CN107406438A

CN107406438A - The inhibitor of bromine domain

Info

Publication number: CN107406438A
Application number: CN201580066751.6A
Authority: CN
Inventors: O·哈伦科; P·R·扬; S·D·布朗; B·C·杜菲; S·刘; P·古佐
Original assignee: Zinneth Epigenetics Ltd
Current assignee: Hengyi Biomedicine Shanghai Co ltd
Priority date: 2014-12-17
Filing date: 2015-12-16
Publication date: 2017-11-28
Anticipated expiration: 2035-12-16
Also published as: EP3233846A1; JP2017538721A; US20170360760A1; CN107406438B; HK1245247A1; EP3233846A4; WO2016097863A1; US10231953B2; CA2966450A1

Abstract

The present invention relates to the compound for the covalency inhibitor for potentially acting as bromine domain and the therapeutical uses of these inhibitor.

Description

The inhibitor of bromine domain

It is described this application claims the priority for the U.S. Provisional Application No. 62/093,394 submitted on December 17th, 2014 Application is incorporated herein in entirety by reference.

The present invention provide compounds, the pharmaceutical composition containing this kind of compound and its in prevention and treatment and bromine Purposes in the domain disease and the patient's condition relevant with additional terminals domain (BET) protein.

Gene expression and the regulation of chromatin organization are related to the posttranslational modification (PTM) of histone in eukaryotic.In spy It is exactly by histone acetyltransferases (HAT) and deacetylase (HDAC) tune to determine the acetylation of histone at lysine residue The PTM of section.Peserico, A. and C.Simone, " physics and feature HAT/HDAC interaction regulatory protein matter acetylations are put down Weigh (Physical and functional HAT/HDAC interplay regulates protein acetylation Balance) ",《Biomedical and biotechnology magazine (J Biomed Biotechnol)》, 2011：371832(2011).Just HDAC and HAT micromolecular inhibitor is being studied as cancer therapy.Hoshino, I. and H.Matsubara, " histone takes off second Latest developments (the Recent advances in histone deacetylase targeted of acyl enzyme target on cancer therapy cancer therapy)”《Surgery today (Surg Today)》40(9)：809-15(2010)；Vernarecci, S., F.Tosi and P.Filetici, " with HAT inhibitor adjustment acetylation chromatin：A kind of novel therapeutic instrument (Tuning acetylated chromatin with HAT inhibitors：a novel tool for therapy)”《Test embryo Learn (Epigenetics)》5(2)：105-11(2010)；Bandyopadhyay, K. et al., " the HAT suppressions based on spermidine CoA Inhibitor Blocks DNA is repaired and is provided cancer specific chemotherapy sensitizing and radiosensitization (Spermidinyl-CoA-based HAT inhibitors block DNA repair and provide cancer-specific chemo-and Radiosensitization) ",《Cell cycle (Cell Cycle)》8(17)：2779-88(2009)；Arif, M. et al., " cell function of protein lysine acetylation and its effect (Protein lysine in cancer displays Acetylation in cellular function and its role in cancer manifestation) ",《Biology Chemistry and Acta Biophysica Sinica (Biochim Biophys Acta)》1799(10-12)：702-16(2010).Histone acetyl Change and the protein complex of acetylated lysine is bonded directly to by bromine domain to control gene expression by raising. Sanchez, R. and M.M.Zhou, " effect (The role of mankind's bromine domain in chromatin biology and genetic transcription Of human bromodomains in chromatin biology and gene transcription) ",《Drug discovery Newly see (Curr Opin Drug Discov Devel) with exploitation》12(5)：659-65(2009).One such family's bromine structure Domain and additional terminals domain (BET) protein include Brd2, Brd3, Brd4 and BrdT, its each containing two series connection can be only On the spot it is attached to the bromine domain of acetylated lysine, such as Wu, S.Y. and the C.M.Chiang, " chromatin containing double bromine domains Conjugant Brd4 and transcriptional regulatory (The double bromodomain-containing chromatin adaptor Brd4 And transcriptional regulation) ",《Journal of biological chemistry (J Biol Chem)》282(18)：13141-5 (2007) summarized in.

BET protein interactions are disturbed to adjust usually the transcription journey relevant with disease by suppressing bromine domain Sequence, the disease are characterised by that cell cycle control, expression of inflammatory cytokines, virus transcription, hematopoietic differentiation, insulin turn Record and fat generation dysregulation.Belkina, A.C. and G.V.Denis, " the BET domains in fat, inflammation and cancer The auxiliary adjustment factor (BET domain co-regulators in obesity, inflammation and cancer) ", 《Natural cancer summarizes (Nat Rev Cancer)》12(7)：465-77(2012).Think BET inhibitor be applied to treatment with Systemic or tissue inflammation, the inflammatory reaction to infection or anoxic, cell activation are related to propagation, lipid-metabolism, fibrosis Disease or the patient's condition, and suitable for prevention and treatment virus infection.Belkina, A.C. and G.V.Denis, " fat, inflammation and The BET domain auxiliary adjustments factor in cancer ",《Natural cancer summary》12(7)：465-77(2012)；Prinjha, R.K., J.Witherington and K.Lee, " your BET is put well：Treatment potential (the Place your BETs of bromine domain： The therapeutic potential of bromodomains) ",《Pharmaceutical science trend (Trends Pharmacol Sci)》33(3)：146-53(2012).

Autoimmune disease is often chronic and makes one weak, is the result of immune response imbalance, and immune response is lost Tune causes physical aggression cell, tissue and the organ of its own.Pro-inflammatory cytokine includes IL-1 β, TNF-α, IL-6, MCP- 1 and IL-17, is overexpressed in autoimmune disease.IL-17 expresses the T cell subgroup for defining referred to as Th17 cells, its part Ground is broken up by IL-6, and has been promoted many in the pathogenic consequence of autoimmune disease.Therefore, IL-6/Th17 axles represent The important potential pharmacy target spot in autoimmune disease therapy.Kimura, A. and T.Kishimoto, " IL-6：Treg/ Regulatory factor (the IL-6 of Th17 balances：Regulator of Treg/Th17 balance) ",《European Journal of Immunology (Eur J Immunol)》40(7)：1830-5(2010).It is expected that BET inhibitor has anti-inflammatory and immuno-modulating properties.Belkina, A.C. and G.V.Denis, " the BET domain auxiliary adjustments factor in fat, inflammation and cancer ",《Natural cancer summary》12 (7)：465-77(2012)；Prinjha, R.K., J.Witherington and K.Lee, " put your BET well：Bromine domain is controlled Treat potential ",《Pharmaceutical science trend》33(3)：146-53(2012).BET inhibitor shown with the external antiinflammation of wide spectrum, Including reducing such as expression in the immunocyte activated of IL-1 β, MCP-1, TNF-α and IL-6 pro-inflammatory cytokines Ability.Mirguet, O. et al., " it is transferred to BET families bromine domain from ApoAl to suppress：I-BET151 discovery (From ApoAl upregulation to BET family bromodomain inhibition：discovery of I- BET151) ",《Bioorganic Chemistry and medical chemistry communication (Bioorg Med Chem Lett)》22(8)：2963-7 (2012)；Nicodeme, E. et al., " suppress inflammation (Suppression of by the histone analogies of synthesis Inflammation by a synthetic histone mimic) ",《Natural (Nature)》468(7327)：1119-23 (2010)；Seal, J. et al., " differentiate the novel series of BET families bromine domain inhibitor：I-BET151(GSK1210151A) Binding pattern and overview (Identification of a novel series of BET family bromodomain inhibitors：Binding mode and profile of I-BET151 (GSK1210151A)) ",《Bioorganic Chemistry Communicated with medical chemistry》22(8)：2968-72(2012).The mechanism of these antiinflammations can be related to BET inhibitor and destroy NF- The Brd4 co-activations and/or BET protein of the pro-inflammatory cytokine of κ B regulations are from cytokine promoter (including IL-6) It is mobile.Nicodeme, E. et al., " suppressing inflammation by the histone analogies of synthesis ",《It is natural》468(7327)：1119-23 (2010)；Zhang, G. et al., " downward NF- κ B transcriptional activities (Down- is suppressed by BRD4 in the related nephrosis of HIV regulation of NF-kappaB Transcriptional Activity in HIVassociated Kidney Disease by BRD4Inhibition) ",《Journal of biological chemistry》, 287 (34)：8840-51(2012)；Zhou, M. et al., " bromine domain protein white matter Brd4 by threonine 29 phosphorylation CDK9 come adjust human immunodeficiency virus transcribe (Bromodomain protein Brd4 regulates human immunodeficiency virus Transcription through phosphorylation of CDK9 at threonine 29) ",《Journal of Virology (J Virol)》83(2)：1036-44(2009).In addition, because Brd4 take part in T cell lineage, BET inhibitor can be with Suitable for the inflammatory conditions characterized by the specific program that T cell is broken up.Zhang, W.S. et al. the, " egg of brominated domain Phosphorylation (the Bromodomain- of rna plymerase ii serine 2 in white matter 4 (BRD4) regulation mankind's CD4+T cells Containing-Protein 4(BRD4)Regulates RNA Polymerase II Serine 2 Phosphorylation in Human CD4+T Cells) ",《Journal of biological chemistry》(2012).

The anti-inflammatory and immunoregulation effect that BET suppresses also have been confirmed in vivo.In mouse, BET inhibitor prevents The death that the death and cecal ligation and perforation that endotoxin or bacterial septicemia induce induce, indicates BET inhibitor and is losing Effectiveness in terms of mass formed by blood stasis and acute inflammatory illness.Nicodeme, E. et al., " suppress scorching by the histone analogies of synthesis Disease ",《It is natural》468(7327)：1119-23(2010).It has been shown that the animal model HIV-1 transgenosis in HIV associated kidney diseases is small In mouse, BET inhibitor improves inflammation and kidney injury partially by the interaction for suppressing Brd4 and NF- κ B.Zhang, G. et al., " suppress to lower NF- κ B transcriptional activities (the Down-regulation of NF- in HIV associated kidney diseases by BRD4 kappaB Transcriptional Activity in HIV associated Kidney Disease by BRD4Inhibition) ",《Journal of biological chemistry》287(34)：8840-51(2012).In mouse multiple sclerosis model Demonstrate BET and suppress the effectiveness in autoimmune disease, wherein BET suppresses to draw partially by IL-6 and IL-17 is suppressed The clinical sign for playing disease eliminates.R.Jahagirdar, S.M. et al., " in mouse multiple sclerosis model, oral biology Available small molecule RVX-297 significantly reduces disease (An Orally Bioavailable Small Molecule RVX- 297 Significantly Decreases Disease in a Mouse Model of Multiple Sclerosis) ", 《World's inflammation meeting (World Congress of Inflammation)》, Paris, FRA (Paris, France) (2011). These results have obtained the support of similar mouse model, are shown in similar mouse model, are handled with BET inhibitor and inhibit T Cells in vitro, which is divided into, promotees autoimmune T h1 and Th17 subgroup, and further obviates what is induced by proinflammatory Th1 cells Disease.Bandukwala, H.S. et al., " by BET protein and c-Myc inhibitor selective depression CD4+T cells because Son produces and LADA (Selective inhibition of CD4+T-cell cytokine production and Autoimmunity by BET protein and c-Myc inhibitors) ",《NAS proceeding (Proc NatlAcad Sci USA)》109(36)：14532-7(2012).

BET inhibitor goes for treating the inflammatory patient's condition of various chronic auto-immunes.Therefore, of the invention one Aspect provides compound, composition and the method for treating LADA and/or diseases associated with inflammation, and methods described is to pass through Administration one or more the compounds of this invention or the pharmaceutical composition comprising one or more of those compounds.It can use The LADA and diseases associated with inflammation of Compounds and methods for treatment, the example of illness and syndrome of the present invention is included (but not Be limited to) inflammatory pelvic disease, urethritis, skin sunburn, nasosinusitis, pneumonia, encephalitis, meningitis, myocarditis, ephritis (Zhang, G. et al., " suppressing to lower the NF- κ B transcriptional activities in HIV associated kidney diseases by BRD4 ",《Journal of biological chemistry》 287(34)：8840-51(2012))；Osteomyelitis, myositis, hepatitis, gastritis, enteritis, dermatitis, gingivitis, appendicitis, pancreatitis, Cholecystitis, agammaglobulinemia, psoriasis, allergy, Crohn's disease (Crohn ' s disease), knot intestines easily swash synthesis Sign, ulcerative colitis (Prinjha, R.K., J.Witherington and K.Lee, " put your BET well：Bromine domain is controlled Treat potential ",《Pharmaceutical science trend》33(3)：146-53(2012))；Sjogren syndrome (Sjogren ' s disease), group Knit graft-rejection, the hyperacute rejection of transplant organ, asthma, allergic rhinitis, chronic obstructive pulmonary disease (COPD), Autoimmune polyglandular disease (also referred to as autoimmune polyglandular syndrome), LADA baldness, pernicious anaemia, kidney are small Ball ephritis, dermatomyositis, multiple sclerosis (Bandukwala, H.S. et al., " pass through BET protein and c-Myc inhibitor Selective depression CD4+T cell cytokines produce and LADA ",《NAS's proceeding》109(36)： 14532-7(2012))；Chorionitis, vasculitis, Autoimmune hemolytic and thrombocytopenic state, Gourde(G) Paasche Che Shi Syndrome (Goodpasture ' s syndrome), atherosclerosis, Addison's disease (Addison ' s disease), pa Gold gloomy sick (Parkinson ' s disease), Alzheimer disease (Alzheimer ' s disease), type i diabetes (Belkina, A.C. and G.V.Denis, " the BET domain auxiliary adjustments factor in fat, inflammation and cancer ",《Natural cancers Disease is summarized》12(7)：465-77(2012))；Septic shock (Zhang, G. et al., " suppresses to lower HIV correlation kidneys by BRD4 NF- κ B transcriptional activities in disease ",《Journal of biological chemistry》287(34)：8840-51(2012))；Systemic lupus erythematosus (SLE) (Prinjha, R.K., J.Witherington and K.Lee, " put your BET well：The treatment potential of bromine domain ",《Medicine section Trend》33(3)：146-53(2012))；Rheumatoid arthritis (Denis, G.V., " cancer, obesity, diabetes B and inflammation The bromine domain co-activating factor (Bromodomain coactivators in cancer, obesity, type in disease 2diabetes, and inflammation) ",《Drug discovery (Discov Med)》10(55)：489-99(2010))；Ox-hide Tinea arthritis, juvenile arthritis, osteoarthritis, chronic idiopathic thrombocytopenic purpura, the huge balls of Walden Si Telun Proteinemia (Waldenstrom macroglobulinemia), myasthenia gravis, Hashimoto's thyroiditis (Hashimoto ' s Thyroiditis), atopic dermatitis, degenerative joint disease, leucoderma, LADA hypopituitarism, Ji Lan-Ba Lei Syndrome (Guillain-Barre syndrome), Behcet's disease (Behcet ' s disease), uveitis, scheroma, sclerderm Disease, mycosis fungoides and Graves disease (Graves ' disease).

BET inhibitor goes for treating the various acute inflammatory patient's condition.Therefore, one aspect of the present invention provides use In compound, composition and the method for the treatment of the inflammatory patient's condition, the inflammatory patient's condition includes but is not limited to acute gout, kidney Scorching including lupus nephritis, the vasculitis for thering is organ to participate in, such as glomerulonephritis, vasculitis including giant cell arteritis, Wei Lattice receive granulomatosis (Wegener ' s granulomatosis), PAN, Behcet's disease, Kawasaki disease (Kawasaki ) and takayasu's arteritis (Takayasu ' s arteritis) disease.

BET inhibitor goes for prevention and treatment and is related to directed toward bacteria, virus, fungi, parasite and its toxin sense The disease or the patient's condition of the inflammatory reaction of dye, such as (but not limited to) septicemia, sepsis syndrome, septic shock (Nicodeme, E. et al., " suppressing inflammation by the histone analogies of synthesis ",《It is natural》468(7327)：1119-23 (2010)), systemic inflammatory response syndrome (SIRS), multiple organ dysfunction syndrome, TSS, acute Injury of lungs, adult respiratory distress syndrome (ARDS) (ARDS), acute renal failure, fulminant hepatitis, burn, Post-operative syndrome, sarcoid Disease, herxheimer reaction (Herxheimer reaction), encephalitis, myelitis, meningitis, malaria and relevant with viral infection SIRS, such as influenza, herpes zoster, herpes simplex and coronavirus.Belkina, A.C. and G.V.Denis, " fat, inflammation With the BET domain auxiliary adjustments factor in cancer ",《Natural cancer summary》12(7)：465-77(2012).Therefore, this hair Bright one side provide for treat directed toward bacteria as described herein, virus, fungi, parasite and its toxi-infection these Compound, composition and the method for inflammatory reaction.

Cancer is one group of disease as caused by the cell propagation lacked of proper care.Therapy approach is intended to by suppressing cellular replication or logical Induction Carcinoma cell differentiation or death are crossed to reduce the quantity of cancer cell, but also meets the medical treatment to more effective therapeutic agent far away Demand.Cancer cell have accumulated heredity and epigenetic change, and these changes change cell growth and metabolism, promote cell increasing Grow and improve the resistance to apoptosis or Apoptosis.Some of these changes includes tumor suppressor gene Inactivation, oncogene activation and chromatin Structure regulation change, include histone PTM imbalance.Watson, J.D., " ' can not be cured ' cancer (Curing ' incurable ' cancer) is cured ",《Cancer finds (Cancer Discov)》1(6)：477-80(2011)；Morin, R.D. et al., " the histone modification gene in non Hodgkin lymphom Frequent mutation (Frequent mutation of histone-modifying genes in non-Hodgkin lymphoma)”《It is natural》476(7360)：298-303(2011).

One aspect of the present invention provides compound, composition and the method for treating human cancer, the cancer bag Include (but not limited to) cancer as caused by the anomalous translocation or overexpression of BET protein (such as NUT center line cancers (NMC) (French, C.A., " NUT center line cancers (NUT midline carcinoma) ",《Cancer genet and cytogenetics (Cancer Genet Cytogenet)》203(1)：16-20 (2010)) and B cell lymphoma (Greenwald, R.J. et al., " E mu-BRD2 transgenic mices develop B cell lymphoma and leukaemia (E mu-BRD2 transgenic mice develop B-cell lymphoma and leukemia) ",《Blood (Blood)》103(4)：1475-84(2004))).Brd4 or Brd3 Group translocation NMC growth of tumour cell to the gene drivings of nutlin 1.Filippakopoulos, P. et al., " selectivity suppression BET bromines domain (Selective inhibition of BET bromodomains) processed ",《It is natural》468(7327)： 1067-73(2010).BET suppresses to demonstrate potent antitumor activity in NMC muroid heteroplastic transplantation model, and NMC is one Kind is rare, but the cancer of lethal form.The present invention provides a kind of method for treating human cancer, and the cancer includes Cancer of the (but not limited to) depending on the myc family members of oncoprotein, the member include c-myc, MYCN and L- myc.Vita, M. and M.Henriksson, " therapy target (The Myc of the Myc cancer proteins as human cancer Oncoprotein as a therapeutic target for human cancer) ",《Carcinobiology seminar (Semin Cancer Biol)》16(4)：318-30(2006).These cancers include Burkitt's lymphoma (Burkitt ' s Lymphoma), acute myelogenous leukemia, Huppert's disease and aggressive mankind's medulloblastoma.Vita, M. and M.Henriksson, " therapy target of the Myc cancer proteins as human cancer ",《Carcinobiology seminar》16(4)：318-30 (2006).The cancer that c-myc is overexpressed is particularly susceptible to the influence of BET protein suppression；It has been proved that with BET inhibitor The tumour of c-myc activation is treated by making c-myc transcriptional inactivations cause tumor regression.Dawson, M.A. et al., " suppress BET Raise effective treatment (Inhibition of BET recruitment to of the chromatin as MLL- fusion leukaemia Chromatin as an effective treatment for MLL-fusion leukaemia) ",《It is natural》478 (7370)：529-33(2011)；Delmore, J.E. et al., " BET bromines domain suppresses the therapeutic strategy as targeting c-Myc (BET bromodomain inhibition as a therapeutic strategy to target c-Myc) ",《Cell (Cell)》146(6)：904-17(2010)；Mertz, J.A. et al., " by suppressing the MYC in BET bromine domain target on cancer Dependence (Targeting MYC dependence in cancer by inhibiting BET bromodomains) ", 《NAS's proceeding》108(40)：16669-74(2011)；Ott, C.J. et al., " BET bromines domain suppresses targeting C-Myc and IL7R (BET bromodomain inhibition in excessive risk acute lymphoblastic leukemia Targets both c-Myc and IL7R in highrisk acute lymphoblastic leukemia) ",《Blood》 120(14)：2843-52(2012)；Zuber, J. et al., " RNAi screenings differentiate Brd4 as in acute myelogenous leukemia Therapy target (RNAiscreen identifies Brd4as a therapeutic target in acute myeloid Leukaemia) ",《It is natural》478(7370)：524-8(2011).

Embodiments of the invention include being used to treat following method：Dependent on BET protein and pTEFb (Cdk9/ cells Cyclin T) adjust the human cancer of oncogene (Wang, S. and P.M.Fischer, " cyclin dependent kinase Enzyme 9：Key transcription regulatory factor and potential drug target spot (Cyclin- in oncology, virology and cardiology dependent kinase 9：a key transcriptional regulator and potential drug target In oncology, virology and cardiology) ",《Pharmaceutical science trend》29(6)：302-13 (2008)), and can With by suppressing Bcl2, cell cycle protein dependent kinase 6 (CDK6) (Dawson, M.A. et al., " suppression BET recruitment dyeing Effective treatment of the matter as MLL- fusion leukaemia ",《It is natural》478(7370)：529-33 (2011)), or human telomerase reverse is inverse Transcriptase (hTERT) (Delmore, J.E. et al., " BET bromines domain suppresses the therapeutic strategy as targeting c-Myc ",《Carefully Born of the same parents》146(6)：904-17(2010)；Ruden, M. and the N.Puri, " novel anti-cancer therapy (Novel of Targeting Telomerase Anticancer therapeutics targeting telomerase) ",《(Cancer Treat are summarized in treatment of cancer Rev)》39(5)：444-456 (2012)) cancer coming inducing cell apoptosis or aging and treat.

The increasing of the known drive transducer relevant with some human diseases teiology can also be caused by suppressing BET protein Suppression (Hnisz, D. et al. " control cell identity and the super enhancer (Super- of disease of hadron and/or super enhancer Enhancers in the control of cell identity and disease) ",《Cell》155：934-947 (2013)；Loven, J. et al. are " by destroying super enhancer selective depression tumour oncogene (Selective inhibition of tumor oncogenes by disruption of super-enhancers.)”《Cell》153： 320-334(2013)；" main transcription factor and amboceptor establish super enhancing at key cells identity gene by Whyte, W.A. et al. Son (Master transcription factors and mediator establish super-enhancers at key Cell identity genes) ",《Cell》153：307-319(2013)).MYC oncogene be with by BET- bromine domains The example for the relevant gene of super enhancer that inhibitor destroys.See, for example, Loven (2013).Therefore, of the invention one Aspect provides compound, composition and the method for treating such disease and illness, the disease and illness include with can be with With the relevant cancer of the super enhancer or enhancer of the destruction of BET inhibitor.

BET inhibitor goes for treating cancer, and the cancer includes but is not limited to adrenal, acinar cells Cancer, acoustic neurinoma, acral lentiginous melanoma, acrospiroma, acute eosinophilic leukemia, acute red white blood Disease, acute lymphoblastic leukemia (see, for example, Loven (2013)), acute megakaryoblastic leukaemia, acute list Monocytic leukemia, acute myelogenous leukemia (Dawson, M.A. et al., " suppress BET recruitment chromatin as MLL- to melt Close effective treatment of leukaemia ",《It is natural》478(7370)：529-33(2011)；Mertz, J.A. et al., " by suppressing BET MYC dependences (Targeting MYC dependence in cancer by bromine domain target on cancer Inhibiting BET bromodomains) ",《NAS's proceeding》108(40)：16669-74(2011)； Zuber, J. et al., " RNAi screenings differentiate Brd4 as the therapy target in acute myelogenous leukemia ",《It is natural》478 (7370)：524-8 (2011)), gland cancer, adenoid cystic carcinoma, adenoma, Odontogenic cysts adenoid tumour, adenosquamous carcinoma, adipose tissue anything superfluous or useless, Adrenocortical carcinoma, adult T-cell leukemia/lymthoma (Wu, X. et al. " bromine domain and additional terminals domain (BET) protein Suppress to have contained human T-leukemia virus 1 (HTLV-1) Tax albumen by suppressing Nuclear factor kappa B (NF- κ B) signal transduction The tumour of matter mediation forms (Bromodomain and extraterminal (BET) protein inhibition suppresses human T cell leukemia virus 1(HTLV-1)Tax protein-mediated Tumorigenesis by inhibiting nuclear factor kappaB (NF-kappaB) signaling) ",《Biology The Chemicals》288：36094-36105 (2013)), aggressive NK chronic myeloid leukemias, AIDS associated lymphomas, acinus shape band Muscle tumor, alveolar soft part sarcoma, ameloblastic fibroma, primary cutaneous type, undifferentiated thyroid carcinoma, blood vessel (Knoechel, B. et al. " are treated immunoblastic t cell lymphoma in T cell acute lymphoblastic leukemia to targeting Epigenetic mechanism (the An epigenetic mechanism of resistance to targeted of the resistance of method Therapy in T cell acute lymphoblastic leukemia) ",《Natural science of heredity (Nat Genet)》46： 364-370(2014)；Loosveld, M. et al. are " in therapeutic targeting T cell acute lymphoblastic leukemia (T-ALL) C-Myc (Therapeutic Targeting of c-Myc in T-Cell Acute Lymphoblastic Leukemia (T-ALL)) ",《Tumor targets (Oncotarget)》5(10)：3168-72(2014)；Reynolds, C. et al. " is in excessive risk T In cell acute lymphoblastic leukaemia, BIM suppression mediates survival-signal to conduct (Repression by MYC and AKT of BIM mediates survival signaling by MYC and AKT in high-risk T-cell acute Lymphoblastic leukemia) ",《Leukaemia (Leukemia)》28(9)：1819-27(2014)；Roderick, J.E. Et al. " c-Myc suppress prevent in mouse trigger leukaemia and weaken recurrent and induce failure paediatrics T-ALL cells Growth (c-Myc inhibition prevents leukemia initiation in mice and impairs the Growth of relapsed and induction failure pediatric T-ALL cells) ",《Blood》123： 1040-1050 (2014)), angiomyoliopma, angiosarcoma, astrocytoma, atypia monster sample Rhabdoid tumor, B it is thin (Ott, C.J. et al., " it is acute thin into lymph that BET bromines domain suppresses targeting excessive risk to born of the same parents' acute lymphoblastic leukemia C-Myc and IL7R (BET bromodomain inhibition targets both c-Myc and in born of the same parents' property leukaemia IL7R in highrisk acute lymphoblastic leukemia) ",《Blood》120(14)：2843-52(2012))、 B cell chronic lymphocytic leukemia, B cell pre-lymphocytic leukemia, B cell lymphoma (Greenwald, R.J. Et al., " E mu-BRD2 transgenic mices develop B cell lymphoma and leukaemia (E mu-BRD2transgenic mice Develop B-cell lymphoma and leukemia) ",《Blood》103(4)：1475-84 (2004)), basal cell Cancer, cancer of bile ducts, carcinoma of urinary bladder, enblastoma, osteocarcinoma (Lamoureux, F. et al. " selective depression BET bromine domain epigenetics Malignancy of tumor circulation (the Selective inhibition of BET bromodomain that signal transduction interference bone photo closes epigenetic signalling interferes with the bone-associated tumour vicious Cycle) ",《Naturally (Nature Comm) is communicated》5：3511 (2014)), brenner tumor (Brenner tumor), brown Knurl, Burkitt's lymphoma (Mertz, J.A. et al., " by suppressing the MYC dependences in BET bromine domain target on cancer (Targeting MYC dependence in cancer by inhibiting BET bromodomains) ",《State of the U.S. The academy of sciences of family proceeding》108(40)：16669-74 (2011)), (Feng, Q. et al. " are used for TAM resistance mammary gland to breast cancer Apparent gene group approach (the An epigenomic approach to therapy for tamoxifen- of the therapy of cancer Resistant breast cancer) ",《Cell research (Cell Res)》24：809-819(2014)；Nagarajan, S. etc. People " bromine domain protein white matter BRD4 is (Bromodomain needed for the activation of ERs dependence enhancer and genetic transcription Protein BRD4 Is Required for Estrogen Receptor-Dependent Enhancer Activation And Gene Transcription) ",《Cell reports (Cell Rep)》8：460-469(2014)；Shi, J. et al. " are destroyed The interaction that BRD4 reverses with diacetylation inhibits the tumour in substrate sample breast cancer to form (Disrupting the Interaction of BRD4with Diacetylated Twist Suppresses Tumorigenesis in Basal- Like Breast Cancer) ",《Cancer cell (Cancer Cell)》25：210-225 (2014)), the cancer of the brain, carcinoma, carcinoma in situ, Carcinosarcoma, cartilage tumor, cementoma, medullary system sarcoma, chondroma, chordoma, choriocarcinoma, papilloma choroideum, kidney are transparent Cell sarcoma, craniopharyngioma, skin T cell lymphoma, cervical carcinoma, colorectal cancer, degos' disease (Degos disease), Desmoplastic small round cell tumor, diffusivity large B cell lymphoid tumor (Chapuy, B. et al. " diffusivity large B cell The discovery of the related dependence of super enhancer and sign (Discovery and characterization of in lymthoma Super-enhancer-associated dependencies in diffuse large B cell lymphoma) ",《Cancer Cell》24：777-790(2013)；Trabucco, S.E. et al. " suppress bromine domain protein white matter to treat the big B of mankind's diffusivity Cell lymphoma (Inhibition of bromodomain proteins for the treatment ofhuman Diffuse large B-cell lymphoma) ",《Clinical Cancer Research (Clin Can Res)》21(1)：113-122 (2015)；Ceribelli, M. et al. " block diffusivity large B cell by bromine domain and additional terminals domain protein inhibitor Carcinogenicity I kappa b kinases activity (Blockade of oncogenic IkappaB kinase activity in lymthoma diffuse large B-cell lymphoma by bromodomain and extraterminal domain protein Inhibitors) ", PNAS 111：11365-11370 (2014)), dysontogenesis nerve epithelioma, dysgerminoma, Embryonal carcinoma, incretory anything superfluous or useless, endodermal sinus tumor, enteropathy associated T cell lymthoma, the cancer of the esophagus, fetus in fetu, fibroma, fibre Tie up sarcoma, follicular lymphoma, follicular thyroid carcinoma, ganglioma, human primary gastrointestinal cancers, germinoma, gestational choriocarcinoma, Megaloblastic desmocytoma, giant cell tumor of bone, neuroglial tumor, glioblastoma multiforme (Cheng, Z et al. " suppression target gene variation spongioblastoma (the Inhibition of BET bromodomain of BET bromine domains Targets genetically diverse glioblastoma) ",《Clinical Cancer Research》19：1748-1759(2013)； " BET bromine domain proteins white matter is (BET bromodomain needed for spongioblast oncocyte propagation by Pastori, C. et al. Proteins are required for glioblastoma cell proliferation) ",《Experimental embryology》9∶ 611-620 (2014)), glioma, gliomatosis cerebri, glucagonoma of pancreas, gonadoblastoma, granulosa cell tumor, Two gonadoblastomas, gallbladder cancer, stomach cancer, hairy cell leukemia, hemangioblastoma, head and neck cancer, hemangiopericytoma, blood Malignant diseases, hepatoblastoma, liver and spleen t cell lymphoma, hodgkin's lymphomas, non Hodgkin lymphom (Lwin, T. etc. People " the c-Myc/miR-548m/HDAC6 amplifications loop (A of the microenvironment mediation in non-Hodgkin's B cell lymphoma microenvironment-mediated c-Myc/miR-548m/HDAC6 amplfication loop in non- Hodgkin B cell lymphomas) ",《Journal of Clinical Investigation (J Clin Invest)》123：4612-4626(2013))、 Aggressive lobular carcinoma, intestinal cancer, kidney, laryngocarcinoma, lentigo maligna, lethal midline cancer, leukaemia, Leydig cell tumour It is (Leydig cell tumor), embryonal-cell lipoma, lung cancer, lymphangioma, lymphangioendothelial sarcoma, lymphoepithelioma, lymthoma, acute Lymphocytic leukemia, acute myelogenous leukemia (Mertz, J.A. et al., " by suppressing BET bromine domain target on cancer In MYC dependences (Targeting MYC dependence in cancer by inhibiting BET Bromodomains) ",《NAS's proceeding》108(40)：16669-74 (2011)), the white blood of chronic lymphocytic (" human lung adenocarcinoma cell is to the apparent something lost of BET by Lockwood, W.W. et al. for disease, liver cancer, ED-SCLC, non-small cell lung cancer Pass sensitiveness (the Sensitivity of human lung adenocarcinoma of the targeted inhibition of signal transduction protein Cell lines to targeted inhibition of BET epigenetic signaling proteins) ", PNAS 109：19408-19413(2012)；" BET bromines domain suppresses in Kras mutability non-small cell lungs by Shimamura, T. et al. The effect of in cancer (Efficacy of BET bromodomain inhibition in Kras-mutant non-small Cell lung cancer) ",《Clinical Cancer Research》19：6183-6192 (2013)), MALT lymthomas, malignant fibrous histiocytoma (" PRC2 loses the Ras signal transductions being exaggerated in cancer by Baude, A. et al. for cytoma, Malignant Peripheral Nerve Sheath Tumours (PRC2loss amplifies Ras signaling in cancer) ",《Natural genetics》46：1154-1155 (2014)；" BET bromines domain suppresses to trigger the related pernicious peripheral nerve sheaths of NF1 by Bim inductions by Patel, A.J. et al. Apoptosis (the BET bromodomain inhibition triggers apoptosis of NF1- of tumour Associated malignant peripheral nerve sheath tumors through Bim induction) ", 《Cell is reported》6：81-92 (2014)), triton tumor, lymphoma mantle cell (Moros, A. et al. " lenalidomide and BET bromines Synergistic antitumor activity (Synergistics of the domain inhibitor C PI203 in bortezomib resistance lymphoma mantle cell antitumor activity of lenalidomide with the BET bromodomain inhibitor CPI203in bortezomib-resistant mantle cell lymphoma) ",《Leukaemia》28∶2049-2059 (2014)), marginal zone B-cell lymphoma, mast cell leukemia, Germ Cell Tumors of Mediastinum, medullary carcinoma of breast, medullary thyroid Sample cancer, medulloblastoma (Bandopadhayay, P. et al. " BET bromine domains of the medulloblastoma of MYC amplifications Suppress (BET bromodomain inhibition of MYC-amplified medulloblastoma) ",《Clinical cancer Research》20：912-925(2014)；" it is medulloblastoma that BET bromine domain proteins white matter, which suppresses, by Henssen, A.G. et al. Therapeutic choice (BET bromodomain protein inhibition is a therapeutic option for medulloblastoma)”《Tumor targets》4(11)：2080-2089(2013)；" BET bromines domain suppresses by Long, J. et al. Agent I-BET151 is worked in smooth downstream to eliminate growth (the The BET bromodomain of hedgehog driving cancer inhibitor I-BET151acts downstream of Smoothened to abrogate the growth of Hedgehog driven cancers) ",《Journal of biological chemistry》289(51)：35494-35502(2014)；Tang, Y. et al. " epigenetic is suppressed by BET bromines domain and targets hedgehog path transcription output (Epigenetic targeting of Hedgehog pathway transcriptional output through BET bromodomain inhibition) ", 《Natural medicine (Nat Med)》20(7)：732-40(2014)；" BRD4 suppression reduces swollen by Venataraman, S. et al. Oncocyte self-renewing and inhibit MYC drive medulloblastoma in stem cell signal transduction (Inhibition of BRD4 attenuates tumor cell self-renewal and suppresses stem cell signaling in MYC driven medulloblastoma) ",《Tumor targets》5(9)：2355-71 (2014)), melanoma (Segura et al., " BRD4 is novel therapeutic target spot (the BRD4is a novel therapeutic target in melanoma Melanoma) ",《Cancer research》72(8)：Supplementary issue 1 (2012)), meningioma, Merkel cell cancer (Merkel cell Cancer), celiothelioma, metastatic bladder transitional cell carcinoma, seedling Le type mixed tumour (mixed Mullerian tumor), mixed stocker are white Blood disease (Dawson, M.A. et al., " suppress BET and raise effective treatment of the chromatin as MLL- fusion leukaemia ",《It is natural》 478(7370)：529-33 (2011)), mucinous tumors, Huppert's disease (Delmore, J.E. et al., " BET bromine domains Suppress the therapeutic strategy as targeting c-Myc ",《Cell》146(6)：904-17 (2010)), musculature anything superfluous or useless, gill fungus sample fungi Disease, myxoid liposarcoma, myxoma, myxosarcoma, nasopharyngeal carcinoma, neurinoma, neuroblastoma (Puissant, A. etc. People " suppresses MYCN (the Targeting MYCN in targeting neuroblastoma by BET bromines domain Neuroblastoma by BET bromodomain inhibition) ",《Cancer is found》3：308-323(2013)；Wyce, Et al. A. " in neuroblastoma tumor model, BET suppresses to make MYCN and BCL2 expression silencing and induces cytotoxicity (BET inhibition silences expression of MYCN and BCL2and induces cytotoxicity in neuroblastoma tumor models)”.《Public science library integrates (PLoS One)》8：e72967 (2014)), neurofibroma, neuroma, nodular melanoma, NUT center line cancers (Filippakopoulos, P. et al., " selection Property suppress BET bromines domain (Selective inhibition of BET bromodomains) ",《It is natural》468(7327)： 1067-73 (2010)), cancer eye, less dash forward astrocytoma, oligodendroglioma, oncocytoma, vagina nervi optici meninx (" selective depression BET bromine domains epigenetic is believed by Lamoureux, F. et al. for knurl, optic nerve tumors, carcinoma of mouth, osteosarcoma The malignancy of tumor circulation that number Conduction Interference bone photo closes "《Naturally communicate》5：3511(2014)；Lee, D.H. et al. " are used to treat The JQ1 of human bone osteosarcoma and cooperative effect (the Synergistic effect of JQ1 and rapamycin of rapamycin For treatment of human osteosarcoma) ",《International journal of cancer (Int J Cancer)》136(9)： 2055-2064 (2014)), oophoroma, pancoast's tumor (Pancoast tumor), papillary thyroid carcinoma, Chromaffionoma, Pineoblastoma, pinealocytoma, pituicytoma, pituitary adenoma, pituitary tumor, plasmacytoma, polyembryoma, precursor T lymphoblastic lymphomas, primary central nervous system lymphoma, lymphoma primary effusion (Tolani, B. et al. " with Myc (the Targeting Myc in lymphoma primary effusion related BET bromine domains inhibitor targeting KSHV KSHV-associated primary effusion lymphoma with BET bromodomain inhibitors) ", 《Oncogene (Oncogene)》33：2928-2937 (2014)), Primary peritoneal carcinoma, prostate cancer (Asangani, I.A. etc. People " BET bromine domain proteins white matter (the Therapeutic targeting of BET in treatment targeting castration refractory prostate cancer Bromodomain proteins in castration-resistant prostate cancer), "《It is natural》510：278- 282(2014)；" the novel GEM models RapidCaP for being used for metastatic prostate cancer analysis and therapy is disclosed by Cho, H. et al. Pusher (RapidCaP, a novel GEM model for metastatic that myc shifts as Pten mutant Prostate cancer analysis and therapy, reveals myc as a driver of Pten-mutant Metastasis) ",《Cancer is found》4∶318-333(2014)；" androgen receptor is raised by c-Myc to be promoted by Gao, L. et al. Prostate cancer process (the Androgen receptor promotes ligand-independent prostate of part independence Cancer progression through c-Myc upregulation) ",《Public science library integrates》8： e63563(2013)；Wyce, A. et al. " therapy approach of the suppression of BET bromine domain protein white matters as prostate cancer (Inhibition of BET bromodomain proteins as a therapeutic approach in prostate Cancer) ",《Tumor targets》4：2419-2429 (2013)), cancer of pancreas (Sahai, V. et al. " BET bromine domains inhibitor hinder Growth (the BET bromodomain inhibitors block growth of of pancreatic cancer cell in disconnected three dimensional collagen Pancreatic cancer cells in three-dimensional collagen) ",《Molecule treatment of cancer (Mol Cancer Ther)》13：1907-1917 (2014)), pharynx cancer, pseudodmyxoma peritonei, clear-cell carcinoma, renal medullary carcinoma, into retina Cytoma, rhabdomyoma, rhabdomyosarcoma, Li Xite conversion (Richter ' s transformation), the carcinoma of the rectum, sarcoma, Schwann's cell tumor disease (Schwannomatosis), seminoma, Sertoli cell tumour (Sertoli cell Tumor), sex cords-gonadal stromal tumor, signet ring cell cancer, cutaneum carcinoma, little Lan circles cell tumour, small cell carcinoma, soft tissue meat Knurl, somatostatinoma, soot wart, tumor of spinal cord, splenic marginal zone lymthoma, squamous cell carcinoma, synovial sarcoma, Xi Zeli diseases (Sezary ' s disease), carcinoma of small intestine, carcinoma squamosum, stomach cancer, carcinoma of testis, theca cell tumor, thyroid cancer, migratory cell Cancer, laryngocarcinoma, carcinoma of urachus, genitourinary cancers, bladder transitional cell carcinoma, uveal melanoma, uterine cancer, verrucous carcinoma, regarding logical Road glioma, carcinoma of vulva, carcinoma of vagina, macroglobulinemia Waldenstron, papillary cystadenoma lymphomatosum (Warthin ' s tumor) with And wilms' tumor (Wilms ' tumor).Therefore, one aspect of the present invention provide for treat such cancer compound, Composition and method.

The BET inhibitor of the present invention goes for the treatment cancer resistant to current and following treatment of cancer Disease, because BET protein take part in the resistance mechanism of some anticancer therapies, including (Feng, Q. et al. " are used for him to chemotherapy The not apparent gene group approach of the therapy of former times sweet smell resistant breast cancer "《Cell research》24：809-819 (2014)), immunotherapy (Emadali, A. et al. " differentiate novel BET bromine domain inhibitor：Control the Rituximab in aggressive lymph cancer anti- Should be with sensitive Gene regulation loop (the Identification of a novel BET bromodomain of tumour growth Inhibitor-sensitive, gene regulatory circuit that controls Rituximab response And tumour growth in aggressive lymphoid cancers) ",《European Molecular Biology Organization molecule doctor Learn (EMBO Mol Med)》5：1180-1195 (2013)), hormonal deprivation (Asangani, I.A. et al. " therapeutic targeting BET bromine domain proteins white matter (Therapeutic targeting of BET in castration refractory prostate cancer Bromodomain proteins in castration-resistant prostate cancer) ",《It is natural》510：278- 282 (2014)) or other molecules (Knoechel, B. et al. are " to targeted therapies in T cell acute lymphoblastic leukemia Resistance epigenetic mechanism (An epigenetic mechanism of resistance to targeted Therapy in T cell acute lymphoblastic leukemia) ",《Natural genetics》46：364-370 (2014)).In these cases, BET protein take part in the resistance mechanism of cancer therapy, and handle list with BET inhibitor Combine solely or with other therapies the sensitiveness that can recover to treatment, Inhibit proliferaton or inducing cell death or aging (" lenalidomide is with BET bromines domain inhibitor C PI203 in bortezomib resistance lymphoma mantle cell by Moros, A. et al. Synergistic antitumor activity (Synergistic antitumor activity of lenalidomide with the BET Bromodomain inhibitor CPI203 in bortezomib-resistant mantle cell 1ymphoma) ", 《Leukaemia》28：2049-2059(2014)).

BET inhibitor goes for treating benign proliferative and fibrotic conditions, including benign soft tissue neoplasm, bone swell Knurl, brain and tumor of spinal cord, eyelid and orbital tumor, granuloma, lipoma, meningioma, Multiple Endocrine neoplasia, breath Meat, pituitary tumor, prolactinoma, pseudotumor cerebri, seborrheic keratosis, polyp of stomach, thyroid nodule, pancreas capsule anything superfluous or useless, blood Tuberculation, vocal nodule, polyp and tumour, castleman's disease, chronic pilonidal disease, histiocytoma, pilar cyst, suppurative granulation Swollen, juvenile polyposis syndrome, idiopathic pulmonary fibrosis, kidney fibrosis, postoperative stenosis, keloid are formed, chorionitis with And cardiac fibrosis.Tang, X. et al., " evaluation idiopathic pulmonary fibrosis lung fibroblast in and pulmonary fibrosis In vivo model In Brd4 suppress (Assessment of Brd4 Inhibition in Idiopathic Pulmonary Fibrosis Lung Fibroblasts and in Vivo Models of Lung Fibrosis) ",《American Journal of Pathology (Am J Pathology)》183(2)：470-479(2013).Therefore, one aspect of the present invention is provided for treating such hyperplasia of prostate Compound, composition and the method for property and fibrotic conditions.

In the U.S., the main reason for angiocardiopathy (CVD) is the death rate and the incidence of disease.Roger, V.L. et al., " heart Disease and apoplexy statistics -- update within 2012：Report (Heart disease and stroke from American Heart Association statistics--2012update：A report from the American Heart Association) ",《Circulation (Circulation)》125(1)：e2-e220(2012).CVD potential cause of disease atherosclerosis is with dyslipidemia and inflammation The multi-factor disease that disease is characterized.Because the ability of foregoing antiinflammation and increase HDL key component ApoA-I transcription, It is expected that BET inhibitor is effective in atherosclerosis and related conditions.Mirguet, O. et al., " from ApoA1 BET families bromine domain is transferred to suppress：I-BET151 discovery (From ApoA1 upregulation to BET family bromodomain inhibition：Discovery of I-BET151) ",《Bioorganic Chemistry communicates with medical chemistry》22 (8)：2963-7(2012)；Chung, C.W. et al., " discovery of the micromolecular inhibitor of BET families bromine domain and sign (Discovery and characterization of small molecule inhibitors of the BET Family bromodomains) ",《Pharmaceutical chemistry magazine (J Med Chem)》54(11)：3827-38(2011).Therefore, originally The one side of invention provides compound, composition and the method for treating angiocardiopathy, and the angiocardiopathy includes (but not limited to) atherosclerosis.

Up-regulation ApoA-I is considered as treating atherosclerosis and CVD available strategy.Degoma, E.M. and D.J.Rader, " drug treatment strategies (the Novel HDL-directed pharmacotherapeutic of novel HDL orientations Strategies) ",《Naturally cardiology (NatRev Cardiol) is summarized》8(5)：266-77(2011).It has been shown that BET Inhibitor improves ApoA-I transcriptions and protein expression.Mirguet, O. et al., " BET families bromine structure is transferred to from ApoA1 Domain suppresses：I-BET151 discovery ",《Bioorganic Chemistry communicates with medical chemistry》22(8)：2963-7(2012)；Chung, C.W. et al., " discovery of the micromolecular inhibitor of BET families bromine domain and sign ",《Pharmaceutical chemistry magazine》54(11)： 3827-38(2011).Also show, BET inhibitor is bonded directly to BET protein and suppresses BET protein to be attached to ApoA- Acetylated histones at 1 promoter, show that BET protein in ApoA-1 promoters be present suppresses compound, its function can To be destroyed by BET inhibitor.It follows that BET inhibitor goes for treating lipid generation by adjusting ApoA-I and HDL Decline office, invitation, etc. on account of illness disease, such as hypercholesterolemia, dyslipidemia, atherosclerosis (Degoma, E.M. and D.J.Rader, " novel HDL The drug treatment strategies of orientation ",《Naturally cardiology is summarized》8(5)：266-77 (2011)), and Alzheimer disease and Other nervous disorders.Elliott, D.A. et al. the, " apolipoprotein in brain：Nervous disorders and the hint of psychiatric condition (Apolipoproteins in the brain：implications for neurological and psychiatric Disorders) ",《Clinical blood fat (Clin Lipidol)》51(4)：555-573(2010).Therefore, a side of the invention Face provides a mean for raising ApoA-1 to treat the compound of cardiovascular disorder, composition and method.

BET inhibitor goes for preventing and treating the patient's condition relevant with Ischemia-reperfusion injury, such as (but it is unlimited In) miocardial infarction, apoplexy, acute coronary syndrome (Prinjha, R.K., J.Witherington and K.Lee, " put well Your BET：The treatment potential of bromine domain ",《Pharmaceutical science trend》33(3)：146-53 (2012)), kidney Reperfu- sion damage, Organ transplant, coronary artery bypass grafting, cardiopulmonary bypass program, hypertension, lung, kidney, liver, stomach-intestines or tip limbs embolism.Cause This, one aspect of the present invention is provided for preventing and treating the patient's condition relevant with Ischemia-reperfusion injury as described herein Compound, composition and method.

Fat related inflammation is the mark of type ii diabetes, insulin resistance and other metabolism disorders.Belkina, A.C. And G.V.Denis, " the BET domain auxiliary adjustments factor in fat, inflammation and cancer ",《Natural cancer summary》12(7)： 465-77(2012)；Denis, G.V., " the bromine domain co-activating factor in cancer, obesity, diabetes B and inflammation ",《Medicine Thing is found》10(55)：489-99(2010).It is consistent to suppress the ability of inflammation with BET inhibitor, in mouse, Brd2 gene Destroy the insulin resistance for eliminating inflammation and making animal be induced from obesity.Wang, F. et al., " Brd2 is destroyed in mouse Severe simple obesity (Brd2 disruption in mice causes severe obesity are caused in the case of without diabetes B The diabetes of without Type 2) ",《Journal of biological chemistry (Biochem J)》425(1)：71-83(2010).Show Show, Brd2 and PPAR γ interact and resist its functional transcription.The mesh that weak Brd2 promotes PPAR γ regulations is struck in vitro Transcription, including lipogenetic those meshes of control.Denis, G.V. et al., " protein of brominated domain is in fat Emerging effect (An emerging role for bromodomain- in the chromatin regulation and transcription control of generation containing proteins in chromatin regulation and transcriptional control of Adipogenesis) ",《Federation of European biochemistry association bulletin (FEBSLett)》584(15)：3260-8(2010).This Outside, Brd2 altimeters in pancreatic beta cell reach and adjust propagation and insulin transcription.Wang, F. et al., " Brd2 in mouse Destruction causes severe simple obesity in the case of without diabetes B ",《Journal of biological chemistry》425(1)：71-83(2010).Total For, BET inhibitor reduces insulin resistance to the compound action of inflammation and metabolism and goes for treating sugar early stage Urine disease and type ii diabetes individual and the patient with other Metabolic complications.Belkina, A.C. and G.V.Denis, " fertilizer The BET domain auxiliary adjustments factor in fat, inflammation and cancer ",《Natural cancer summary》12(7)：465-77(2012).Cause This, one aspect of the present invention provides compound, composition and the method for treating and preventing metabolism disorder, and the metabolism is lost Adjust and include but is not limited to fat related inflammation, type ii diabetes and insulin resistance.

BET inhibitor goes for prevention and treatment and is based on episomal DNA virus, the including but not limited to mankind Papillomavirus, herpesviral, Epstein-Barr virus (Epstein-Barr Virus), human immunodeficiency virus (Belkina, A.C. and G.V.Denis, " the BET domain auxiliary adjustments factor in fat, inflammation and cancer ",《Natural cancer Disease is summarized》12(7)：465-77 (2012)), adenovirus, poxvirus, hepatitis B virus and hepatitis C virus.It has been shown that by place The BET protein of main coding is critically important to the transcription activating of viral promotors and suppression.Brd4 and human papilloma virus (HPV) E2 protein interactions, realize E2- target genes E2 mediation transcription.Gagnon, D. et al., " papillomavirus E2 The proteasome of protein is degraded is suppressed (Proteasomal by the overexpression of the protein 4 of brominated domain degradation of the papillomavirus E2protein is inhibited by overexpression of Bromodomain-containing protein 4) ",《Journal of Virology (J Virol)》83(9)：4127-39(2009). Similarly, Brd2, Brd3 and Brd4 are fully incorporated to by the related herpesviral of Kaposi sarcoma (Kaposi ' s sarcoma) (KSHV) the incubation period nuclear antigen 1 (LANA1) of coding, the LANA1 dependences propagation of KSHV infection cells is promoted.You, J. etc. People, " the related herpesviral incubation period correlation nuclear antigen of Kaposi sarcoma and the bromine structure on host's mitotic chromosome Domain PROTEIN B rd4 interactions (Kaposi ' s sarcoma-associated herpesvirus latency- associated nuclear antigen interacts with bromodomain protein Brd4on host Mitotic chromosomes) ",《Journal of Virology》80(18)：8909-19(2006).It has been shown that BET inhibitor suppresses Brd4 mediations raise transcription elongation complex pTEFb to the viral C promoters of Epstein-Barr virus (EBV), show related to EBV The therapeutic value of malignant diseases.Palermo, R.D. et al., " rna plymerase ii, which is stagnated, promotes nucleosome occlusion and pTEFb recruitments (RNA polymerase II stalling promotes nucleosome are immortalized to be driven by Epstein-Barr virus occlusion and pTEFb recruitment to drive immortalization by Epstein-Barr Virus) ",《Public science library pathogen (PLoS Pathog)》7(10)：e1002334(2011).In addition, potential T cell is infected with potential monocyte infection model, and BET inhibitor reactivates HIV, is potentially allowed for by complementary degeneration-resistant Retroviral Therapy eradicates virus.Zhu, J. et al., " potential HIV-1 is set to be re-activated (Reactivation by suppressing BRD4 Of Latent HIV-1by Inhibition of BRD4) ",《Cell is reported》2(4)：807-816(2012)；Banerjee, C. et al., " BET bromines domain suppresses novel strategy (the BET bromodomain inhibition as HIV-1 reactivations As a novel strategy for reactivation of HIV-1) ",《Leukocyte-biological magazine (J Leukoc Biol)》92(6)：1147-1154(2012)；Bartholomeeusen, K. et al., " BET bromines domain suppresses by from 7SK SnRNP transiences release P-TEFb activated transcriptions (BET bromodomain inhibition activates Transcription via a transient release of P-TEFb from 7SK snRNP) ",《Biochemistry is miscellaneous Will》287(43)：36609-36616(2012)；Li, Z. et al., " BET bromines domain inhibitor JQ1 passes through antagonism Tat Transactivations Brd4 suppress and activate latent HIV (The BET bromodomain inhibitor JQ1 activates HIV Latency through antagonizing Brd4 inhibition of Tat-transactivation) ",《Nucleic acid is ground Study carefully (Nucleic Acids Res)》(2012).Therefore, present invention also offers for treating and preventing based on episomal Compound, composition and the method for DNA virus infection.Specifically, one aspect of the present invention is provided for treating and/or pre- The compound of preventing virus infection or the malignant diseases relevant with the infection, composition and method, the virus infection are included (but not It is limited to) by HPV, KSHV, EBV, HIV, HBV, HCV, adenovirus, poxvirus, herpesvirus infection.

Some central nervous system (CNS) diseases are characterized in the illness during epigenetic.By Brd2 haplotypes Deficiency connects with neuron defects and epilepsy.Velisek, L. et al., " GABA serotonergic neuron defects are complete as idiopathic Body epilepsy mechanism：Effect (GABAergic neuron of the BRD2 haploinsufficiencies in teenager's myoclonus epilepsy deficit as an idiopathic generalized epilepsy mechanism：the role of BRD2haploinsufficiency injuvenile myoclonic epilepsy) ",《Public science library integrates (PLoS One)》6(8)：e23656(2011).Also the SNP in the protein of various brominated domains is contacted with phrenoblabia Get up, the phrenoblabia includes schizophrenia and anxiety disorder.Prinjha, R.K., J.Witherington and K.Lee, " put your BET well：The treatment potential of bromine domain ",《Pharmaceutical science trend》33(3)：146-53(2012).Furthermore, it is contemplated that Relation between the increased ApoA-I Ahl tribulus sea silent sickness proposed and other nervous disorders, BET inhibitor increase ApoA- The ability of I transcriptions can cause BET inhibitor suitable for Alzheimer disease therapy.Elliott, D.A. et al., " in brain Apolipoprotein：Nervous disorders and the hint of psychiatric condition ",《Clinical blood fat》51(4)：555-573(2010).Therefore, originally The one side of invention provides compound, composition and the method for treating such CNS diseases and illness.

BRDT is the testes specificity member of BET protein familieses, and it is to the chromatin remodeling during spermiogenesis tail to pass It is important.Gaucher, J. et al., " carry out bromine domain dependence phase specificity male gene group by Brdt to program (Bromodomain-dependent stage-specific male genome programming by Brdt) ",《Europe J. Mol. BioL (EMBO J)》31(19)：3809-20(2012)；Shang, E. et al. the, " albumen containing double bromine domains The testes specificity member Brdt of the BET subfamilies of matter the first bromine domain breaks up most important (The to male germ cell First bromodomain of Brdt, a testis-specific member of the BET sub-family of Double-bromodomain-containing proteins, is essential for male germ cell Differentiation) ",《Develop (Development)》134(19)：3507-15(2007).BRDT heredity is exhausted or led to The interaction for crossing BET inhibitor suppression BRDT and acetylated histones generates contraceptive effect in mouse, when small point of use During sub- BET inhibitor, this effect is reversible.Matzuk, M.M. et al., " little molecules in inhibiting BRDT is so as to male contraception (Small-Molecule Inhibition of BRDT for Male Contraception) ",《Cell》150(4)：673- 684(2012)；Berkovits, B.D. et al., " testis specific protein matter BRDT and multiple spliceosome containing double bromine domains Component formed compound and for the mRNA montages in circular spermatid and 3 '-UTR truncate needed for (The testis- specific double bromodomain-containing protein BRDT forms a complex with multiple spliceosome components and is required for mRNA splicing and 3′-UTR Truncation in round spermatids) ",《Nucleic acids research》40(15)：7162-75(2012).These as shown by data The potential utility of BET inhibitor as novel and effective male contraception approach.Therefore, another aspect of the present invention provides use In the compound of male contraception, composition and method.

Monocyte chemoattractant protein-1 (MCP-1, CCL2) plays an important role in angiocardiopathy.Niu, J. and P.E.Kolattukudy, " effects of the MCP-1 in angiocardiopathy：Molecular mechanism and clinical meaning (Role of MCP-1 in cardiovascular disease：Molecular mechanisms and clinical implications) ", 《Clinical science (Clin Sci)》(London) 117 (3)：95-109(2009).MCP-1 adjusts monocyte by its chemotactic activity Recruitment from lumen of artery to subcutaneous clearance, in subcutaneous clearance, monocyte develops into macrophage foam cells, and triggers The formation of fatty streaks, fatty streaks can develop into atherosclerotic plaque.Dawson, J. et al., " in targeting disease Monocyte chemoattractant protein-1 signal transduction (Targeting monocyte chemoattractant protein-1 Signalling in disease) ",《Therapy target expert opinion (Expert Opin Ther Targets)》7(1)：35- 48(2003).Having checked MCP-1 under hyperlipidemia background in various transgenosis and gene knock-out mice model, (and its is same Source acceptor CCR2) key effect in the evolution of atherosclerosis.Boring, L. et al., " in CCR2-/- mouse Lesion, which forms to reduce, discloses effect (Decreased lesion of the chemotactic factor (CF) in terms of atherosclerosis is triggered formation in CCR2-/-mice reveals a role for chemokines in the initiation of Atherosclerosis) ",《It is natural》394(6696)：894-7(1998)；Gosling, J. et al., " lacking MCP-1 reduces It is overexpressed human apolipoprotein B neurological susceptibility (MCP-1 deficiency reduces of the mouse to atherosclerosis susceptibility to atherosclerosis in mice that overexpress human Apolipoprotein B) ",《Journal of Clinical Investigation》103(6)：773-8(1999)；Gu, L. et al., " monocyte chemotactic egg - 1 shortage reduces atherosclerosis (the Absence of monocyte of LDL receptor deficient mice in vain chemoattractant protein-1 reduces atherosclerosis in low density lipoprotein Receptor-deficient mice) ",《Molecular cell (Mol Cell)》2(2)：275-81(1998)；Aiello, R.J. etc. People, " monocyte chemoattractant protein-1 accelerates the atherosclerosis (Monocyte of Apolipoprotein E-deficient mouse chemoattractant protein-1 accelerates atherosclerosis in apolipoprotein E- Deficient mice) ",《Artery sclerosis, thrombosis and Vascular Biology (Arterioscler Thromb Vasc Biol)》19(6)：1518-25(1999).These reports prove, eliminate MCP-1 signal transductions and cause the macrophage to arterial wall thin Born of the same parents infiltrate reduction and atherosclerotic lesion development weakens.

In the mankind, the correlation between MCP-1 and angiocardiopathy is firmly established.Niu, J. and P.E.Kolattukudy, " effects of the MCP-1 in angiocardiopathy：Molecular mechanism and clinical meaning ",《Clinical science》(human relations Earnestly) 117 (3)：95-109(2009).In human atherosclerosis's patch, endothelial cell, smooth muscle cell and wellability list Nucleus/macrophage is overexpressed MCP-1 and its acceptor.Nelken, N.A. et al., " in human atherosclerosis's patch Monocyte chemoattractant protein-1 (Monocyte chemoattractant protein-1 in human atheromatous Plaques) ",《Journal of Clinical Investigation》88(4)：1121-7(1991).In addition, MCP-1 elevated circulation content and major part The incidence of disease of cardiovascular risk factors, the measured value of coronary atherosclerosis load and coronary heart disease (CHD) is proportionate. Deo, R. et al., " blood plasma monocyte chemoattractant protein-1 content, traditional cardiovascular risk factors and subclinical Atherosclerosis Correlation (Association among plasma levels of monocyte chemoattractant between change Protein-1, traditional cardiovascular risk factors, and subclinical Atherosclerosis) ",《JACC (J Am Coll Cardiol)》44(9)：1812-8(2004). MCP-1 content highest CHD patients are the patients with acute coronary syndrome (ACS).De Lemos, J.A. et al., " between the blood plasma monocyte chemoattractant protein-1 content and Long-term clinical result of the patient with acute coronary syndrome Correlation (Association between plasma levels of monocyte chemoattractant protein- 1 and long-term clinical outcomes in patients with acute coronary Syndromes) ",《Circulation》107(5)：690-5(2003).In addition to being worked in the potential inflammation relevant with CHD, MCP-1, which is also shown, take part in plaque rupture, ischemic/Reperfu- sion damage, ISR and heart transplant rejection.Niu, J. and P.E.Kolattukudv, " effects of the MCP-1 in angiocardiopathy：Molecular mechanism and clinical meaning ",《Clinical science》 (London) 117 (3)：95-109(2009).

MCP-1 further promotes the tissue inflammation relevant with autoimmune disease, including rheumatoid arthritis (RA) and more Hair property sclerosis (MS).MCP-1 works in RA during macrophage and lymphocytic infiltration are into joint, and It is overexpressed in the synovia of RA patient.Koch, A.E. et al., " strengthen and monocyte chemotactic is produced in rheumatoid arthritis (the Enhanced production of monocyte chemoattractant protein-1 in of albumen -1 Rheumatoid arthritis) ",《Journal of Clinical Investigation》90(3)：772-9(1992).Blocked in RA animal model MCP-1 and MCP-1 signal transductions also show that the MCP-1 pairs of accumulation of macrophages relevant with RA and pro-inflammatory cytokine expression Importance.Brodmerkel, C.M. et al., " the novel effective CCR2 antagonists INCB3344 of rodent discovery and medicine Neo-Confucianism characterizes (Discovery and pharmacological characterization of a novel rodent- Active CCR2 antagonist, INCB3344) ",《Journal of Immunology (J Immunol)》175(8)：5370-8(2005)； Bruhl, H. et al., " double actions of the CCR2 during the arthritic initiation and progress that collagen induces：For adjusting Active evidence (the Dual role of CCR2 during initiation and progression of of CCR2+T cells collagen-induced arthritis：evidence for regulatory activity of CCR2+T Cells) ",《Journal of Immunology》172(2)：890-8(2004)；Gong, J.H. et al., it is " single in MRL-lpr mouse models The antagonist of Monocyte chemoattractant protein 1 (MCP-1) suppresses arthritis (An antagonist of monocyte chemoattractant protein 1(MCP-1)inhibits arthritis in the MRL-lpr mouse Model) ",《The Journal of Experimental Medicine (J Exp Med)》186(1)：131-7(1997)；65.Gong, J.H. et al., " use group Suppress muroid arthritis (Post-onset inhibition of murine after closing the breaking-out of chemokine antagonists therapy Arthritis using combined chemokine antagonist therapy) ",《Rheumatology (Rheumatology)》(Oxford 43 (1)：39-42(2004).

In the mankind, overexpressions of the MCP-1 in brain, celiolymph (CSF) and blood is also relevant with chronic and acute MS. Mahad, D.J. and R.M.Ransohoff, " MCP-1 (CCL2) and CCR2 are in multiple sclerosis and experimental autoimmune Effect (The role of MCP-1 (CCL2) and CCR2 in multiple sclerosis in encephalomyelitis (EAE) And experimental autoimmune encephalomyelitis (EAE)) ",《Immunology investigation text volume (Semin Immunol)》15(1)：23-32(2003).MCP-1 during progression of disease by brain various cell types be overexpressed and The infiltration of macrophage and lymphocyte is facilitated, the infiltration mediates the tissue damage relevant with MS.Itself exempt from experimentally In epidemic disease encephalomyelitis (EAE) mouse model (model for being similar to mankind MS), MCP-1 or CCR2 heredity, which are exhausted, to be produced to disease The resistance of disease, is primarily due to reduce CNS macrophages infiltration.Fife, B.T. et al., " CC-chemokine receptor 2 is right Most important (the is critical of CC chemokine receptor 2 of induction of experimental autoimmune encephalomyelitis For induction of experimental autoimmune encephalomyelitis) ",《The Journal of Experimental Medicine》 192(6)：899-905(2000)；Huang, D.R. et al., " lacking MCP 1 in mouse causes experimentally Local macrophage in Autoimmune Encephalomyelitis is raised and the type immune response of antigen specific T auxiliary cell 1 is reduced (Absence of monocyte chemoattractant protein 1 in mice leads to decreased local macrophage recruitment and antigen-specific T helper cell type 1 immune Response in experimental autoimmune encephalomyelitis) ",《The Journal of Experimental Medicine》193(6)： 713-26(2001)。

Preclinical data it has been shown that MCP-1 and CCR2 small molecule and macromolecular inhibitor have as inflammatory and The potential of the therapeutic agent of LADA indication.Therefore, one aspect of the present invention is provided for treating and MCP-1 and CCR2 Relevant cardiovascular, inflammatory and the LADA patient's condition compound, composition and method.

Therefore, the present invention, which provides, is applied to suppress the compound of BET protein functions, bag by being attached to bromine domain Disease is being treated and prevented containing the pharmaceutical composition of one or more of those compounds and these compounds or composition With the purposes in terms of the patient's condition, the disease and the patient's condition include but is not limited to cancer, autoimmunity disease and angiocardiopathy.

One aspect of the present invention, which provides, includes Formulas I and Formula II compound：

And its stereoisomer, dynamic isomer, pharmaceutically acceptable salt and hydrate,

Wherein：

R₁Selected from optionally by 1 to 5 independently selected from R₅Group substitution carbocyclic ring (C₅-C₁₀) and heterocycle (C₂-C₁₀)；

R₂And R₃Independently selected from the alkyl (C optionally substituted by halogen and hydroxyl₁-C₆), its condition is if R₂And R₃It is first Base, then R₁Different from following：

Wherein A is selected from hydrogen, halogen, methoxyl group ,-CN ,-NO₂,-C (O) OMe and-C (O) NMe₂；

R₄If it is present, it is selected from hydrogen, optionally by 1 to 5 independently selected from R₅Group substitution alkyl (C₁-C₁₀)、 Carbocyclic ring (C₃-C₁₀) and heterocycle (C₂-C₁₀)；

Each R₅Independently selected from deuterium, epoxides, alkyl (C₁-C₆) (such as methyl, ethyl, propyl group, isopropyl, butyl), alcoxyl Base (C₁-C₆) (such as methoxyl group, ethyoxyl, isopropoxy), amino (such as-NH₂、-NHMe、-NHEt、-NHiPr、-NHBu、- NMe₂、NMeEt、-NEt₂,-NEtBu) ,-NHC (O) NH- alkyl (C₁-C₆), halogen (such as F, Cl), acid amides (as-NHC (O) Me ,- NHC(O)Et、-C(O)NHMe、-C(O)NEt₂、-C(O)NiPr)、-CF₃、-CN、-N₃, ketone (C₁-C₆) (such as acetyl group ,-C (O) Et ,-C (O) Pr) ,-S (O)-alkyl (C₁-C₄) (such as-S (O) Me ,-S (O) Et) ,-SO₂- alkyl (C₁-C₆) (such as-SO₂Me、- SO₂Et、-SO₂Pr), sulfanyl (C₁-C₆) (as-SMe ,-SEt ,-SPr ,-SBu) ,-COOH and ester (such as-C (O) OMe ,-C (O) OEt ,-C (O) OBu), it each can be optionally by oxirane, hydrogen, F, Cl, Br ,-OH ,-NH₂、-NHMe、-OMe、- SMe, oxo and/or thioxo-oxo substitution；

X is selected from optionally by 1 to 2 independently selected from R₅Group substitution-CH₂-；

Y is if it is present, be selected from-N- ,-CH- and-C (NH₂)-；And

Z is if it is present, selected from hydrogen and amino (such as-NH₂、-NHMe、-NMe₂)。

In another aspect of the present invention, there is provided a kind of pharmaceutical composition, it includes Formulas I or Formula II compound or it is vertical Body isomers, dynamic isomer, pharmaceutically acceptable salt or hydrate, and one or more pharmaceutically acceptable supporting agents, Diluent or excipient.

In another aspect of the present invention, there is provided a kind of Formulas I or Formula II compound or its stereoisomer, tautomerism Body, pharmaceutically acceptable salt or hydrate, it is applied to therapy, especially treats the disease that bromine domain inhibitor is applicable Or the patient's condition.Therefore, one aspect of the present invention is included to mammal in need (for example, mankind) administration therapeutically effective amount Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or hydrate.

Another aspect of the present invention provides the Formulas I to mammal in need (for example, mankind) administration therapeutically effective amount Or Formula II compound or its stereoisomer, dynamic isomer, the method for pharmaceutically acceptable salt or hydrate.

Another aspect of the present invention provides Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically The use of acceptable salt or hydrate in the medicine of the disease being applicable for treatment bromine domain inhibitor or the patient's condition is manufactured On the way.

Brief description of the drawings

Fig. 1 shows covalent compound 5- (dimethyl -1,2- oxazole -4- bases) -1- (the fluoro- 4- of 3- (oxirane -2- bases) benzene Methyl) pyridine -2 (1H) -one (example 1) and 6- (dimethyl -1,2- oxazole -4- bases) -1- { [4- (oxirane -2- bases) benzene Base] methyl -1H-1,3- benzodiazole -4- amine (example 4) compared to non-covalent control removing breed, shown covalent knot Close on breeding persistent influence (example 9).By MV4-11 cells covalency inhibitor and non-covalent control treatment 24 hours, it Compound is removed afterwards and is replaced with culture medium.24,48 and 72 hours after removing, measurement cell propagation.

Fig. 2 displays 5- (dimethyl -1,2- oxazole -4- bases) -1- (the fluoro- 4- of 3- (oxirane -2- bases) benzyl) pyridine - Influence of the covalent bond of 2 (1H) -one (example 1) to MYC and BCL2.By MV4-11 cells covalency inhibitor and non-covalent right According to processing 4 hours, compound was removed afterwards and is replaced with culture medium.4,6 and 24 hours after removing, cell is collected, and Determine MYC and BCL2 expression.

Fig. 3 show thermal migration analysis, present 5- (dimethyl -1,2- oxazole -4- bases) -1- (the fluoro- 4- of 3- (oxirane - 2- yls) benzyl) pyridine -2 (1H) -one (example 1) and 6- (dimethyl -1,2- oxazole -4- bases) -1- { [4- (oxirane -2- Base) phenyl] methyl } -1H-1,30 minutes and 4 hours, time dependence formed covalently multiple 3- benzodiazole -4- amine (example 4) Compound.

Definition

As used in this specification, following word, phrase and symbol are typically intended with implication as hereinbefore set forth, but Except situation indicated otherwise in their context.Abbreviation and term have indicated implication in the whole text below.

As used herein, " angiocardiopathy " refer to by BET suppress mediation heart and the disease of the circulatory system, illness and The patient's condition.Exemplary angiocardiopathy including cholesterol or lipid-associated disorders includes but is not limited to acute coronary syndromes Sign, angina pectoris, artery sclerosis, atherosclerosis, Carotid Atherosclerosis, cranial vascular disease, cerebral infarction, the congested heart Force failure, congenital heart disease, coronary heart disease, coronary artery disease, coronary plaque static stabilization, dyslipidemia, exception Lipoproteinemia, endothelial dysfunction, familial hypercholesterolemia, familial combined hyperlipidemiam, low alpha-lipoprotein blood Disease, hypertriglyceridema, high beta-lipoproteinemia, hypercholesterolemia, hypertension, hyperlipidemia, Charcot's syndrome, lack Blood, ischemic damage and reperfusion damage, ischemic heart disease, heart ischemia, metabolic syndrome, multiple infarct dementia, cardiac muscle stalk Plug, the damage of obesity, peripheral vascular disease, Reperfu- sion, ISR, atherosclerosis of renal artery, rheumatic heart disease, in Wind, thrombotic disorder, the lipoprotein abnormalities that transient ischemic is broken out and Ahl tribulus sea silent sickness is relevant, obesity, diabetes, X Syndrome and impotence.

As used herein, " diseases associated with inflammation " refers to disease, illness and the patient's condition for suppressing mediation by BET.Exemplary inflammation Property disease includes but is not limited to late period and chronic solid after arthritis, asthma, dermatitis, psoriasis, cystic fibrosis, transplanting Organ rejection response, multiple sclerosis, systemic lupus erythematosus, IBD, autoimmune diabetes, diabetic keratopathy PVR, diabetic nephropathy, diabetic angiopathy change, inflammation of eye section, uveitis, rhinitis, ischemia-reperfusion Property damage, postangioplasty restenosis, chronic obstructive pulmonary disease (COPD), glomerulonephritis, Graves disease, intestines and stomach Allergy, conjunctivitis, atherosclerosis, coronary artery disease, angina pectoris and small artery disease.

As used herein, " cancer " refers to disease, illness and the patient's condition for suppressing mediation by BET.Exemplary cancer include (but It is not limited to) chronic lymphocytic leukemia and Huppert's disease, follicular lymphoma, there is centrum germinativum's phenotype more It is denatured between unrestrained property large B cell lymphoid tumor, Burkitt's lymphoma, hodgkin's lymphomas, follicular lymphoma and activation big Cell lymphoma, neuroblastoma and primary nervous ectoderm tumour, rhabdomyosarcoma, prostate cancer, breast cancer, NMC (NUT center line cancers), acute myelogenous leukemia (AML), acute B lymphoblastic leukemia (B-ALL), Bai Jiteshi lymphs Knurl, B cell lymphoma, melanoma, mixed stocker leukaemia, Huppert's disease, promyelocytic leukemia (PML), Fei Huoqi Golden lymphomas, neuroblastoma, medulloblastoma, lung cancer (NSCLC, SCLC) and colon cancer.

" subject " refers to as or by as treatment, the animal of the object of observation or experiment, such as mammal.Herein Described method goes for both human therapy and veterinary application.In one embodiment, subject is the mankind.

As used herein, " treatment (treatment) " or " treatment (treating) " refer to disease or illness or its at least A kind of improvement of recognizable symptom.In another embodiment, " treat (treatment) " or " treatment (treating) " is Refer to the improvement of physical parameter that is at least one measurable but can not necessarily being distinguished by patient.In another embodiment, " treatment (treatment) " or " treatment (treating) " refers to the progress for physically suppressing disease or illness, such as distinguishable The stabilization of other symptom；Or from the progress for physiologically suppressing disease or illness, such as the stabilization of physical parameter；Or both all Have.In another embodiment, " treatment (treatment) " or " treatment (treating) " refers to postpone disease or illness Breaking-out.For example, reduction blood cholesterol levels can be included by treating cholesterol disorders.

As used herein, " prevention (prevention) " or " prevention (preventing) " refer to reduce must specify disease or The risk of illness.

It is not used for the tie point for representing substituent in two short stroke ("-") between letter or symbol.For example ,- CONH₂Connected by carbon atom.

" optional " or " optionally " mean that then described event or situation can occur or can not occur, and institute State the bright situation including event or situation generation and situation about not occurring.For example, " aryl being optionally substituted " is contained Cover " aryl " and " substituted aryl ", defined below.One of ordinary skill in the art it will be appreciated that on it is any containing The group of one or more substituents, these groups be not intended to introduce it is any it is spatially unrealistic, can not in synthesis Row and/or unstable substitution itself or substitute mode.

As used herein, term " hydrate " refers to have stoichiometry or non-stoichiometric water to be incorporated into crystal structure Crystal form.

As used herein, term " alkenyl " refers to the unsaturated straight or branched hydrocarbon with least one carbon-to-carbon double bond, such as The straight or branched group of 2-8 carbon atom, herein referred as (C₂-C₈) alkenyl.Exemplary alkenyl includes but is not limited to ethene Base, pi-allyl, cyclobutenyl, pentenyl, hexenyl, butadienyl, pentadienyl, hexadienyl, 2- ethyl hexyls alkenyl, 2- third Base -2- cyclobutenyls and 4- (2- methyl -3- butylene)-pentenyl.

As used herein, term " alkoxy " refers to the alkyl (- O- alkyl -) being connected with oxygen." alkoxy " also include with The alkenyl (" alkenyloxy group ") of oxygen connection or the alkynyl (" alkynyloxy group ") being connected with oxygen.Exemplary alkoxy including but not limited to contains The alkyl of 1-8 carbon atom, the group of alkenyl or alkynyl, herein referred as (C₁-C₈) alkoxy.Exemplary alkoxy is included (but not It is limited to) methoxyl group and ethyoxyl.

As used herein, term " alkyl " refers to saturated straight chain or branched-chain hydrocarbons, such as the straight or branched base of 1-8 carbon atom Group, herein referred as (C₁-C₈) alkyl.Exemplary alkyl include but is not limited to methyl, ethyl, propyl group, isopropyl, 2- methyl isophthalic acids- Propyl group, 2- methyl-2-propyls, 2-methyl-1-butene base, 3- methyl isophthalic acids-butyl, 2- methyl -3- butyl, 2,2- dimethyl -1- third Base, 2- methyl-1-pentenes base, 3- methyl-1-pentenes base, 4- methyl-1-pentenes base, 2- methyl -2- amyl groups, 3- methyl -2- amyl groups, 4- first Base -2- amyl groups, 2,2- dimethyl -1- butyl, 3,3- dimethyl -1- butyl, 2- ethyl -1- butyl, butyl, isobutyl group, tertiary fourth Base, amyl group, isopentyl, neopentyl, hexyl, heptyl and octyl group.

As used herein, term " alkynyl " refers to the unsaturated straight or branched hydrocarbon with least one carbon-to-carbon triple bond, such as The straight or branched group of 2-8 carbon atom, herein referred as (C₂-C₈) alkynyl.Exemplary alkynyl includes but is not limited to acetylene Base, propinyl, butynyl, pentynyl, hexin base, methylpropynyl, 4- methyl isophthalic acids-butynyl, 4- propyl group-valerylene base and 4- butyl -2- hexin bases.

As used herein, term " acid amides " is finger version-NR_aC(O)(R_b)-or-C (O) NR_bR_c, wherein R_a、R_bAnd R_cRespectively From independently selected from alkyl, alkenyl, alkynyl, aryl, aralkyl, cycloalkyl, alkylhalide group, heteroaryl, heterocyclic radical and hydrogen.Acid amides Carbon, nitrogen, R can be passed through_bOr R_cIt is connected to another group.Acid amides can also be ring-type, for example, R_bAnd R_cIt can connect Connect to form 3 to 8 yuan of rings, such as 5 or 6 yuan of rings.Term " acid amides " covers following group：As sulfonamide, urea, urea groups, carbamate, Carbamic acid and its annular form.Term " acid amides " is also contemplated by the amide groups being connected with carboxyl, such as-acid amides-COOH or salt, Such as-acid amides-COONa；The amino (for example ,-amino-COOH or salt, such as-amino-COONa) being connected with carboxyl.

As used herein, term " amine " or " amino " are finger version-NR_dR_eOr-N (R_d)R_e-, wherein R_dAnd R_eIndependently select From alkyl, alkenyl, alkynyl, aryl, aralkyl, carbamate, cycloalkyl, alkylhalide group, heteroaryl, heterocycle and hydrogen.Amino Parent molecular group can be connected to by nitrogen.Amino can also be ring-type, for example, R_dAnd R_eIn any two can To link together or be linked together with N, 3 to 12 yuan of rings (for example, morpholinyl or piperidyl) are formed.Term amino also includes The corresponding quaternary ammonium salt of any amino.Exemplary amino includes alkylamino, wherein R_dOr R_eIn it is at least one be alkyl.At some In embodiment, Rd and Re each optionally can be substituted by hydroxyl, halogen, alkoxy, ester or amino.

As used herein, term " aryl " refers to monocyclic carbocyclic ring, two carbocyclic rings or other more aromatic ring carbon loop systems.Aryl can Optionally to be condensed with one or more rings selected from aryl, cycloalkyl and heterocyclic radical.The present invention aryl can by selected from Under group substitution：Alkoxy, aryloxy group, alkyl, alkenyl, alkynyl, acid amides, amino, aryl, aralkyl, carbamate, carboxylic Base, cyano group, cycloalkyl, ester, ether, formoxyl, halogen, alkylhalide group, heteroaryl, heterocyclic radical, hydroxyl, ketone, nitro, phosphate, sulphur Compound, sulfinyl, sulfonyl, sulfonic acid, sulfonamide and thioketones.Exemplary aryl include but is not limited to phenyl, tolyl, Anthryl, fluorenyl, indenyl, azulenyl and naphthyl, and benzo-fused isocyclic part, such as 5,6,7,8- tetralyls.Exemplary virtue Base also includes but is not limited to monocyclic aromatic loop system, and its middle ring includes 6 carbon atoms, herein referred as " (C₆) aryl ".

As used herein, the alkyl that term " aralkyl " refers to have at least one aryl substituent is (for example ,-aryl-alkane Base -).Exemplary aralkyl includes but is not limited to the aralkyl with monocyclic aromatic loop system, and its middle ring includes 6 carbon originals Son, herein referred as " (C₆) aralkyl ".

As used herein, term " carbamate " is finger version-R_gOC(O)N(R_h)-、-R_gOC(O)N(R_h)R_i- or-OC (O)NR_hR_i, wherein R_g、R_hAnd R_iIt is each independently selected from alkyl, alkenyl, alkynyl, aryl, aralkyl, cycloalkyl, alkylhalide group, miscellaneous Aryl, heterocyclic radical and hydrogen.Exemplary carbamate includes but is not limited to aryl-carbamate or heteroaryl amino first Acid esters is (for example, wherein R_g、R_hAnd R_iIn it is at least one independently selected from aryl or heteroaryl, such as pyridine, pyridazine, pyrimidine and pyrrole Piperazine).

As used herein, term " carbocyclic ring " refers to aryl or cycloalkyl.

As used herein, term " carboxyl " refers to-COOH or its corresponding carboxylate (for example ,-COONa).Term carboxyl Also include " carboxycarbonyl ", such as the carboxyl being connected with carbonyl, such as-C (O)-COOH or salt, such as-C (O)-COONa.

As used herein, term " cyano group " refers to-CN.

As used herein, term " cycloalkyloxy " refers to the cycloalkyl being connected with oxygen.

As used herein, term " cycloalkyl " refer to 3-12 carbon or 3-8 carbon saturation or unsaturated cyclic, it is bicyclic or The bicyclic alkyl of bridging, the herein referred as " (C derived from cycloalkane₃-C₈) cycloalkyl ".Exemplary cycloalkyl includes but is not limited to Hexamethylene, cyclohexene, pentamethylene and cyclopentene.Cycloalkyl can use following substitution：Alkoxy, aryloxy group, alkyl, alkenyl, alkynes Base, acid amides, amino, aryl, aralkyl, carbamate, carboxyl, cyano group, cycloalkyl, ester, ether, formoxyl, halogen, alkyl halide Base, heteroaryl, heterocyclic radical, hydroxyl, ketone, nitro, phosphate, sulfide, sulfinyl, sulfonyl, sulfonic acid, sulfonamide and sulphur Ketone.Cycloalkyl can condense with other cycloalkyl saturations or unsaturated aryl or heterocyclic radical.

As used herein, term " dicarboxylic acids " refers to the group containing at least two carboxylic acid groups, such as saturation and unsaturated hydrocarbons Dicarboxylic acids and its salt.Exemplary dicarboxylic acids includes alkyl dicarboxylic aid.Dicarboxylic acids can use following substitution：Alkoxy, aryloxy group, alkane Base, alkenyl, alkynyl, acid amides, amino, aryl, aralkyl, carbamate, carboxyl, cyano group, cycloalkyl, ester, ether, formoxyl, Halogen, alkylhalide group, heteroaryl, heterocyclic radical, hydrogen, hydroxyl, ketone, nitro, phosphate, sulfide, sulfinyl, sulfonyl, sulfonic acid, Sulfonamide and thioketones.Dicarboxylic acids include but is not limited to succinic acid, glutaric acid, adipic acid, suberic acid, decanedioic acid, azelaic acid, Maleic acid, phthalic acid, aspartic acid, glutamic acid, malonic acid, fumaric acid, (+)/(-)-malic acid, (+)/ (-) tartaric acid, M-phthalic acid and terephthalic acid (TPA).Dicarboxylic acids further comprises its carboxylic acid derivates, as acid anhydrides, acyl are sub- Amine, hydrazides (for example, succinic anhydride and succimide).

Term " electrophilic group " as described herein is to refer to and amino acid residue (such as cysteine and methionine) Form the functional group of covalent bond.Exemplary electrophilic group include but is not limited to alkylhalide group, epoxides, alkene, acyl halide, Aldehyde, ester, ketone and hydroxyalkyl.In addition, electrophilic group can include the alkyl substituted by following non-limiting group：Halogen (such as Br, Cl, I), epoxides and sulphonic acid ester (such as methanesulfonates, tosylate).

Term " epoxides " refers to oxygen atom and the cyclic ethers of two carbon bond in three-membered ring.Epoxides can be every Optionally at most it is substituted twice on individual carbon atom.Exemplary epoxides include but is not limited to oxirane, expoxy propane, 2,2- dimethyl ethylene oxides and 2,3- dimethyl ethylene oxide.

Term " ester " refers to structure-C (O) O- ,-C (O) O-R_j-、-R_kC(O)O-R_j- or-R_kC (O) O-, wherein O are not bonded To hydrogen, and R_jAnd R_kCan be independently selected from alkoxy, aryloxy group, alkyl, alkenyl, alkynyl, acid amides, amino, aryl, aralkyl Base, cycloalkyl, ether, alkylhalide group, heteroaryl and heterocyclic radical.R_kCan be hydrogen atom, but R_jIt can not be hydrogen atom.Ester can be with It is ring-type, for example, carbon atom and R_j, oxygen atom and R_kOr R_jAnd R_kIt can connect to form 3 to 12 yuan of rings.Exemplary ester At least one in including but not limited to Arrcostab, wherein Rj or Rk is alkyl, such as-O-C (O)-alkyl ,-C (O)-O- alkane Base-and-alkyl-C (O)-O- alkyl-.Exemplary ester is also included in aryl or heteroaryl base ester, such as wherein Rj or Rk at least One is heteroaryl, such as pyridine, pyridazine, pyrimidine and pyrazine, such as nicotinate.Exemplary ester also includes having structure-R_kC(O)O- Anti- ester, wherein oxygen key knot to parent molecule.Exemplary anti-ester includes succinate, D-Arg ester, L-arginine ester, L- and relied Propylhomoserin ester and D-Lys ester.Ester also includes carboxylic acid anhydrides and carboxylic acid halides.

As used herein, term " halogen " or " halogen " refer to F, Cl, Br or I.

As used herein, term " alkylhalide group " refers to the alkyl substituted by one or more halogen atoms." alkylhalide group " is gone back Cover the alkenyl or alkynyl substituted by one or more halogen atoms.

As used herein, term " heteroaryl " refers to containing one or more heteroatomic monocyclic, bicyclic or polycyclic fragrance Race's loop system, such as containing 1-3 hetero atom, such as nitrogen, oxygen and sulphur.Heteroaryl can be substituted with one or more substituents, this One or more substituents include alkoxy, aryloxy group, alkyl, alkenyl, alkynyl, acid amides, amino, aryl, aralkyl, amino first Acid esters, carboxyl, cyano group, cycloalkyl, ester, ether, formoxyl, halogen, alkylhalide group, heteroaryl, heterocyclic radical, hydroxyl, ketone, nitro, phosphorus Acid esters, sulfide, sulfinyl, sulfonyl, sulfonic acid, sulfonamide and thioketones.Heteroaryl can also condense with non-aromatic ring. The illustrative example of heteroaryl includes but is not limited to pyridine radicals, pyridazinyl, pyrimidine radicals, pyrazolyl, triazine radical, pyrrole radicals, pyrrole Oxazolyl, imidazole radicals, (1,2,3)-and (1,2,4)-triazolyl, pyrazinyl, pyrimidine radicals, tetrazole radical, furyl, thienyl, Yi Evil Oxazolyl, thiazolyl, furyl, phenyl, isoxazolyls Yi are Ji oxazolyl.Exemplary heteroaryl includes but is not limited to mono-cyclic aromatic Race's ring, its middle ring include 2-5 carbon atom and 1-3 hetero atom, herein referred as " (C₂-C₅) heteroaryl ".

As used herein, term " heterocycle ", " heterocyclic radical " or " heterocycle " refers to containing one, two or three independently Heteroatomic saturation or unsaturated 3,4,5,6 or 7 yuan of rings selected from nitrogen, oxygen and sulphur.Heterocycle can be aromatic (heteroaryl) Or non-aromatic.Heterocycle can be substituted with one or more substituents, and the one or more substituent includes alkoxy, fragrant oxygen Base, alkyl, alkenyl, alkynyl, acid amides, amino, aryl, aralkyl, carbamate, carboxyl, cyano group, cycloalkyl, ester, ether, first Acyl group, halogen, alkylhalide group, heteroaryl, heterocyclic radical, hydroxyl, ketone, nitro, phosphate, sulfide, sulfinyl, sulfonyl, sulphur Acid, sulfonamide and thioketones.Heterocycle also includes bicyclic, three rings and four cyclic groups, wherein any one in above heterocycle with one Or two rings independently selected from aryl, cycloalkyl and heterocycle condense.Exemplary heterocycle includes acridinyl, benzimidazolyl, benzene And furyl, benzothiazolyl, benzothienyl, benzoxazolyl, biotinyl, cinnolines base, dihydrofuran base, indoline Base, dihydro pyranyl, dihydro-thiophene base, dithiazole base, furyl, homopiperidinyl, imidazolidinyl, imidazolinyl, imidazole radicals, Yin Diindyl base, isoquinolyl, isothiazole alkyl, isothiazolyl, isoxazolidinyl, isoxazolyl, morpholinyl, oxadiazolyl, oxazolidine Ji, oxazolyls, piperazinyl, piperidyl, pyranose, pyrazolidinyl, pyrazinyl, pyrazolyl, pyrazolinyl, pyridazinyl, pyridine radicals, Pyrimidine radicals, pyrimidine radicals, pyrrolidinyl, give a tongue-lashing and cough up alkane -2- ketone groups, pyrrolinyl, pyrrole radicals, quinolyl, quinoxalinyl, tetrahydrofuran Base, tetrahydro isoquinolyl, THP trtrahydropyranyl, tetrahydric quinoline group, tetrazole radical, thiadiazolyl group, thiazolidinyl, thiazolyl, thienyl, Thio-morpholinyl, thiopyranyl and triazolyl.

As used herein, term " hydroxyl (hydroxy) " and " hydroxyl (hydroxyl) " refer to-OH.

As used herein, term " hydroxyalkyl " refers to the hydroxyl being connected with alkyl.

As used herein, term " hydroxyaryl " refers to the hydroxyl being connected with aryl.

As used herein, term " ketone " refers to structure-C (O)-Rn (such as acetyl group-C (O) CH₃) or-R_n-C(O)-R_o-.Ketone R can be passed through_nOr R_oIt is connected to another group.R_nOr R_oCan be alkyl, alkenyl, alkynyl, cycloalkyl, heterocyclic radical or aryl, Or R_nOr R_oIt can connect to form 3 to 12 yuan of rings.

As used herein, term " monoesters " refers to the analog of dicarboxylic acids, one of carboxylic acid functionalised as ester and Another carboxylic acid is free carboxy acid or carboxylate.The example of monoesters includes but is not limited to succinic acid, glutaric acid, adipic acid, pungent Diacid, decanedioic acid, azelaic acid, the monoesters of oxalic acid and maleic acid.

As used herein, term " phenyl " refers to 6 yuan of aromatic ring carbon rings.Phenyl can also be with hexamethylene or pentamethylene ring Fusion.Phenyl can be substituted with one or more substituents, the one or more substituent include alkoxy, aryloxy group, alkyl, Alkenyl, alkynyl, acid amides, amino, aryl, aralkyl, carbamate, carboxyl, cyano group, cycloalkyl, ester, ether, formoxyl, halogen Element, alkylhalide group, heteroaryl, heterocyclic radical, hydroxyl, ketone, phosphate, sulfide, sulfinyl, sulfonyl, sulfonic acid, sulfonamide and Thioketones.

As used herein, term " sulfanyl " refers to the alkyl (- S- alkyl -) being connected with sulphur.

" alkyl ", " alkenyl ", " alkynyl ", " alkoxy ", " amino " and " acid amides " group can be optionally by least one It is individual selected from following group substitution or to be mixed with or branch：Alkoxy, aryloxy group, alkyl, alkenyl, alkynyl, acid amides, amino, aryl, Aralkyl, carbamate, carbonyl, carboxyl, cyano group, cycloalkyl, ester, ether, formoxyl, halogen, alkylhalide group, heteroaryl, heterocycle Base, hydroxyl, ketone, phosphate, sulfide, sulfinyl, sulfonyl, sulfonic acid, sulfonamide, thioketones, urea groups and N.Substituent can Substituted or unsubstituted heterocycle or cycloalkyl are formed with branch.

As used herein, the suitable substitution on the substituent being optionally substituted refers to that the compounds of this invention will not be eliminated The group or intermediate suitable for preparing the compounds of this invention of synthesis or medicinal effectiveness.The example properly substituted is included (but not It is limited to)：C_1-8Alkyl, alkenyl or alkynyl；C_1-6Aryl, C_2-5Heteroaryl；C₃₇Cycloalkyl；C_1-8Alkoxy；C₆Aryloxy group；-CN；- OH；Oxo；Halogen, carboxyl；Amino, such as-NH (C_1-8Alkyl) ,-N (C_1-8Alkyl)₂、-NH((C₆) aryl) or-N ((C₆) virtue Base)₂；Formoxyl；Ketone, such as-CO (C_1-8Alkyl)；-CO((C₆Aryl) ester, such as-CO₂(C_1-8Alkyl) and-CO₂(C₆Aryl).Ability The technical staff in domain can be based on the compounds of this invention stability and pharmacological activity and synthesizing activity and be readily selected conjunction Suitable substitution.

As used herein, term " pharmaceutically acceptable supporting agent " refers to any and all compatible with medicine administration molten Agent, decentralized medium, coating, isotonic agent and absorption delaying agent etc..These media and medicament are in the use of pharmaceutical active substances It is well known in the art.Composition can also contain other reactive compounds, there is provided complementarity, extra or enhancing Treat function.

As used herein, term " pharmaceutically acceptable composition " refer to comprising it is at least one as herein disclosed With the composition for the compound prepared together with one or more pharmaceutically acceptable supporting agents.

As used herein, term " pharmaceutically acceptable prodrug " is represented in the range of rational medical judgment, is applied to Contact with the tissue of the mankind and lower animal and without improper toxicity, stimulation, allergic reaction, match with rational benefit/risk ratio, And in the prodrug of the effective the compounds of this invention of given application, and in the conceived case, the both sexes of the compounds of this invention Ionic species.Higuchi et al., " prodrug (the Prodrugs as Novel Delivery as novel transmission system Systems) ",《Meeting series of books (ACS Symposium Series)》, volume 14 and Roche, E.B. volume《Drug design Bio-reversible supporting agent (Bioreversible Carriers in Drug Design)》, American Pharmaceutical Association (American Pharmaceutical Association) and Pei Geman publishing houses (Pergamon Press), provide discussion in 1987, two Person is incorporated herein by reference.

Term " pharmaceutically acceptable salt " refers to may reside in the acid in compound used in the present composition The salt of property or basic group.In the present composition included property be alkalescence compound can with it is various inorganic and organic Acid forms various salt.The acid for the pharmaceutically acceptable acid-addition salts that can be used for preparing this kind of alkali compounds be to be formed it is nontoxic Acid-addition salts those, i.e. the salt containing pharmaceutically acceptable anion, including but not limited to sulfate, citric acid Salt, malate, acetate, oxalates, chloride, bromide, iodide, nitrate, sulfate, disulfate, phosphate, Acid phosphate, isonicotinic acid salt, acetate, lactate, salicylate, citrate, tartrate, oleate, tannate, Pantothenate, biatrate, ascorbate, succinate, maleate, gentisate, fumarate, glucose It is hydrochlorate, glucuronate, saccharate, formates, benzoate, glutamate, mesylate, esilate, benzene sulfonate, right Toluene fulfonate and embonate (that is, 1,1 '-methylene-bis--(2- hydroxyl -3- naphthoates)).Except being previously mentioned Acid outside, the included compound containing amino part can also form pharmacy with various amino acid in the present composition Upper acceptable salt.In the present composition included property be acid compound can with it is various pharmaceutically acceptable Cation forms alkali salt.The example of this kind of salt includes alkali metal or alkali salt, and especially calcium, magnesium, sodium, lithium, zinc, potassium And molysite.

The compounds of this invention can contain one or more chiral centres and/or double bond, and therefore with stereoisomer Form is present, such as geometric isomer, enantiomter or diastereoisomer.Term " stereoisomer " is as used herein It is made up of all geometric isomers, enantiomter or diastereoisomer.Depending on the substituent around stereogenic carbon atom Configuration, these compounds can use symbol " R " or " S " to represent.The present invention cover these compounds various stereoisomers and Its mixture.Stereoisomer includes enantiomter and diastereoisomer.Enantiomter or diastereoisomer it is mixed Compound can use " (±) " to represent in name, it will be recognized to those skilled in the art that structure can impliedly indicate hand Property center.

The individual stereoisomers of the compounds of this invention can be by synthesis mode by containing asymmetric or cubic symmetry center Commercially available initial substance prepare, it is then well-known by those of ordinary skill in the art or by preparing racemic mixture Method for splitting prepare.These method for splitting are exemplified below：(1) enantiomeric mixture is connected to chiral auxiliary, led to Cross non-enantiomer mixture obtained by recrystallization or chromatographic isolation and discharge optics pure products from auxiliary agent；(2) lived using optics Property resolving agent forming salt；Or (3) separate the mixture of optical enantiomorphs directly on chiral chromatographic column.Crowd can also be passed through Three-dimensional heterogeneous mixture is split into its component stereoisomer by well known method, such as Chiral gas chromatography, chiral high performance liquid Phase chromatogram, make compound crystallization for chiral salt complex or compound is crystallized in chiral solvent.Many institute's weeks can also be passed through The method of asymmetric synthesis known obtains stereoisomer from the pure intermediate of alloisomerism, reagent and catalyst.

There can also be geometric isomer in the compounds of this invention.The present invention covers by the substitution around carbon-to-carbon double bond Various geometric isomers and its mixture caused by the arrangement of base or arrangement around the substituent of carbocyclic ring.Around carbon-to-carbon double bond Substituent " Z " or " E " configuration expression, wherein term " Z " and " E " according to IUPAC standards use.Unless otherwise indicated, it is no The structure for then depicting double bond covers both E and Z isomers.

Around carbon-to-carbon double bond substituent or be properly termed as " cis " or " trans ", wherein it is " cis " expression substituent In the same side of double bond and " trans " expression substituent is in the opposite side of double bond.Arrangement around the substituent of carbocyclic ring is used " suitable Formula " or " trans " expression.Term is " cis " to represent substituent in the same side of plane of a loop and " trans " the expression substituent of term In the opposite side of plane of a loop.Substituent is placed in the same side of plane of a loop and the mixture use of the compound of opposite side is " cis/anti- Formula " represents.

Compound presently disclosed can be existed by tautomeric forms and intend to contain in the scope of the invention Two kinds of tautomeric forms of lid, even if depict only a kind of tautomeric structure.

The exemplary embodiments of the present invention

In some aspects, the present invention relates to a kind of compound according to Formulas I：

Or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or hydrate,

Wherein：

R₄Selected from hydrogen, optionally by 1 to 5 independently selected from R₅Group substitution alkyl (C₁-C₁₀), carbocyclic ring (C₃-C₁₀) with And heterocycle (C₂-C₁₀)；

Each R₅Independently selected from deuterium, epoxides, alkyl (C₁-C₆) (such as methyl, ethyl, propyl group, isopropyl, butyl), alcoxyl Base (C₁-C₆) (such as methoxyl group, ethyoxyl, isopropoxy), amino (such as-NH₂、-NHMe、-NHEt、-NHiPr、-NHBu、- NMe₂、NMeEt、-NEt₂,-NEtBu) ,-NHC (O) NH- alkyl (C₁-C₆), halogen (such as F, C1), acid amides (as-NHC (O) Me ,- NHC(O)Et、-C(O)NHMe、-C(O)NEt₂、-C(O)NiPr)、-CF₃、-CN、-N₃, ketone (C₁-C₆) (such as acetyl group ,-C (O) Et ,-C (O) Pr) ,-S (O)-alkyl (C₁-C₄) (such as-S (O) Me ,-S (O) Et) ,-SO₂- alkyl (C₁-C₆) (such as-SO₂Me、- SO₂Et、-SO₂Pr), sulfanyl (C₁-C₆) (as-SMe ,-SEt ,-SPr ,-SBu) ,-COOH and ester (such as-C (O) OMe ,-C (O) OEt ,-C (O) OBu), it each can be optionally by oxirane, hydrogen, F, Cl, Br ,-OH ,-NH₂、-NHMe、-OMe、- SMe, oxo and/or thioxo-oxo substitution；

X is selected from optionally by 1 to 2 independently selected from R₅Group substitution-CH₂-；And

Y is selected from-N- ,-CH- and-CNH₂-。

In some aspects, the present invention relates to a kind of compound according to Formula II：

Wherein：

R₁Selected from optionally by 1 to 5 independently selected from R₅Group substitution carbocyclic ring (C₅-C₁₀) and heterocycle (C₂-C₁0)；

Z is selected from hydrogen and amino (such as-NH₂、-NHMe、-NMe₂)。

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁Selected from optionally by 1 to 5 independently selected from R₅Group substitution carbocyclic ring (C₅-C₁₀)；And R₂、R₃、R₄、R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁Selected from optionally by 1 to 5 independently selected from R₅Group substitution phenyl；And R₂、R₃、R₄、 R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁Selected from by 1 to 5 independently selected from R₅Group substitution phenyl；And R₂、R₃、R₄、R₅、X、Y And defined in any one or the combination in Z such as this paper paragraphs 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁Selected from by 1 to 5 independently selected from epoxides, alkyl (C₁-C₆) (such as methyl, ethyl, propyl group, Isopropyl, butyl), halogen (such as F, Cl) and ketone (C₁-C₆) (such as acetyl group ,-C (O) Et ,-C (O) Pr) group substitution benzene Base, these groups optionally can each be substituted by oxirane, hydrogen, F, Br and/or Cl；And R₂、R₃、R₄、R₅, X, Y and Defined in any one or combination in Z such as this paper paragraphs 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁Selected from by 1 to 5 groups independently selected from oxirane, methyl, ethyl, F and acetyl group Substituted phenyl, these groups optionally can each be substituted by oxirane and Cl；And R₂、R₃、R₄、R₅, X, Y and Z such as Defined in any one or combination in this paper paragraphs 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁Selected from by oxirane, methyl oxirane, halogen ketone (C₁-C₆) and/or alkylhalide group (C₁-C₆) take The phenyl in generation；And R₂、R₃、R₄、R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁It is selected from：

Wherein benzyl ring is optionally further by 1 to 4 independently selected from R₅Group substitution；And R₂、R₃、R₄、R₅, X, Y with And defined in any one or the combination in Z such as this paper paragraphs 88 to 121.

Wherein benzyl ring is optionally further optionally substituted by halogen；And R₂、R₃、R₄、R₅, X, Y and Z such as this paper paragraphs 88 to 121 In any one or combination defined in.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁It is selected from：Wherein benzyl ring optionally further by 1 to 4 independently selected from R₅Group substitution；And R₂、R₃、R₄、R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁It is selected from：Wherein benzyl ring is optionally further optionally substituted by halogen；And R₂、 R₃、R₄、R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁It is

And R₂、R₃、R₄、R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁Selected from the following group of (but not limited to)：

It is optionally by 1 to 4 independently selected from R₅Group substitution；And R₂、R₃、R₄、R₅, X, Y and Z such as this paper paragraphs Defined in any one or combination in 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁Selected from optionally by 1 to 5 independently selected from R₅Group substitution heterocycle (C₂-C₁₀)；And R₂、R₃、R₄、R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₁Selected from by oxirane, methyl oxirane, halogen ketone (C₁-C₆) and/or alkylhalide group (C₁-C₆) take The 5-6 circle heterocycles in generation；And R₂、R₃、R₄、R₅, determine in any one or combination in X, Y and Z such as this paper paragraph 88 to 121 Justice.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₂It is methyl, and the R in Formulas I and/or Formula II compound₃Selected from optionally being taken by halogen and hydroxyl Alkyl (the C in generation₁-C₆)；And R₁、R₄、R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₂And R₃It is methyl；And R₁、R₄、R₅, in X, Y and Z such as this paper paragraphs 88 to 121 any one or Defined in combination.

In certain embodiments, compound of formula I or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or R in hydrate₄Selected from hydrogen and optionally by 1 to 5 independently selected from R₅Group substitution alkyl (C₁-C₆)；And R₁、 R₂、R₃、R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, compound of formula I or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or R in hydrate₄It is hydrogen；And R₁、R₂、R₃、R₅, institute in any one or combination in X, Y and Z such as this paper paragraph 88 to 121 Definition.

In certain embodiments, compound of formula I or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or R in hydrate₄Selected from optionally by 1 to 5 independently selected from R₅Group substitution alkyl (C₁-C₆)；And R₁、R₂、R₃、 R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₄It is methyl；And R₁、R₂、R₃、R₅, in X, Y and Z such as this paper paragraphs 88 to 121 any one or Defined in combination.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R₄Selected from optionally by 1 to 5 independently selected from R₅Group substitution heterocycle (C₂-C₆)；And R₁、 R₂、R₃、R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in R4 be selected from optionally by 1 to 5 independently selected from R₅Group substitution carbocyclic ring (C₃-C₁₀)；And R₁、R₂、R₃、R₅, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in each R₅Independently selected from deuterium, epoxides, alkyl (C₁-C₆) (such as methyl, ethyl, propyl group, isopropyl Base, butyl), alkoxy (C₁-C₆) (such as methoxyl group, ethyoxyl, isopropoxy), amino (such as-NH₂、-NHMe、-NHEt、- NHiPr、-NHBu、-NMe₂、NMeEt、-NEt₂,-NEtBu) ,-NHC (O) NH- alkyl (C₁-C₆), halogen (such as F, C1), acid amides (such as-NHC (O) Me ,-NHC (O) Et ,-C (O) NHMe ,-C (O) NEt₂、-C(O)NiPr)、-CF₃、-CN、-N₃, ketone (C₁-C₆) (such as Acetyl group ,-C (O) Et ,-C (O) Pr) ,-S (O)-alkyl (C₁-C₄) (such as-S (O) Me ,-S (O) Et) ,-SO₂- alkyl (C₁-C₆) (such as-SO₂Me、-SO₂Et、-SO₂) and sulfanyl (C Pr₁-C₆) (such as-SMe ,-SEt ,-SPr ,-SBu)；And R₁、R₂、R₃、 R₄, defined in any one or combination in X, Y and Z such as this paper paragraph 88 to 121.

In certain embodiments, compound of formula I or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or Y in hydrate is-CH-；And R₁、R₂、R₃、R₄、R₅, in any one or combination in X and Z such as this paper paragraphs 88 to 121 Defined.

In certain embodiments, compound of formula I or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or Y in hydrate is-N-；And R₁、R₂、R₃、R₄、R₅, institute in any one or combination in X and Z such as this paper paragraphs 88 to 121 Definition.

In certain embodiments, compound of formula I or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or Y in hydrate is-C (NH₂)-；And R₁、R₂、R₃、R₄、R₅, any one or group in X and Z such as this paper paragraphs 88 to 121 Defined in conjunction.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in X be-CH₂-, and R₁、R₂、R₃、R₄、R₅, in Y and Z such as this paper paragraphs 88 to 121 any one or Defined in combination.

In certain embodiments, Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt Or the Z in hydrate is hydrogen, and R₁、R₂、R₃、R₄、R₅, in any one or combination in Y and X such as this paper paragraphs 88 to 121 Defined.

In certain embodiments, Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt Or the Z in hydrate is-NH₂, and R₁、R₂、R₃、R₄、R₅, any one or combination in Y and X such as this paper paragraphs 88 to 121 Defined in.

In certain embodiments, Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable Salt or hydrate in epoxides be oxirane, and R₁、R₂、R₃、R₄、R₅, X, Y and Z such as this paper paragraphs 88 to 121 In any one or combination defined in.

In certain embodiments of the present invention, Formula II compound is selected from：

5- (dimethyl -1,2- oxazole -4- bases) -1- (the fluoro- 4- of 3- (oxirane -2- bases) benzyl) pyridine -2 (1H) -one is (real Example 1)；

5- (dimethyl -1,2- oxazole -4- bases) -1- { [4- (oxirane -2- bases) phenyl] methyl } -1,2- dihydropyridines -2- Ketone (example 2)；

3- amino -5- (the different diazole -4- bases of 3,5- dimethyl) -1- (4- (oxirane -2- bases) benzyl) pyridine -2 (1H) -one (example 3)；

And its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or hydrate.

In certain embodiments of the present invention, compound of formula I is selected from：

6- (dimethyl -1,2- oxazole -4- bases) -1- { [4- (oxirane -2- bases) phenyl] methyl } -1H-1,3- benzodiazoles - 4- amine (example 4)；

4- (1- { [4- (2- chloroethyls) phenyl] methyl } -2- methyl isophthalic acid H- imidazos [4,5-b] pyridine -6- bases) -3,5- diformazans Base -1,2- oxazole (example 5)；

The chloro- 1- of 2- (4- { [6- (dimethyl -1,2- oxazole -4- bases) -2- methyl isophthalic acid H- imidazos [4, the 5-b] base of pyridine -1] first Base } phenyl) second -1- ketone (example 6)；

3,5- dimethyl -4- (2- methyl isophthalic acids-{ [4- (oxirane -2- ylmethyls) phenyl] methyl } -1H- imidazos [4,5-b] Pyridine -6- bases) -1,2- oxazoles (example 7)；

And its stereoisomer, dynamic isomer, pharmaceutically acceptable salt and hydrate.

In certain embodiments, such as any one in paragraph 88 to 123 or the Formulas I defined in combination and Formula II chemical combination Thing or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or hydrate can serve as can be with bromine domain protein Amino acid residue (such as cysteine and methionine) at diverse location in white matter forms the electrophilic reagent of covalent bond.

In certain embodiments, by comprising one or more such as any one in paragraph 88 to 123 or defined in combining Formulas I or Formula II II compounds or its stereoisomer, dynamic isomer, the medicine of pharmaceutically acceptable salt or hydrate Composition is configured to transmit by injecting.

Another aspect of the present invention offer is a kind of to suppress the method for BET protein functions by being attached to bromine domain, With its purposes in terms of the disease and the patient's condition of mammal (for example, mankind) is treated and prevented, administration therapeutically effective amount is included Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or hydrate.

In one embodiment, because the strong influence that external BET inhibitor is transcribed on IL-6 and IL-17, BET inhibitor Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or hydrate can Used using being had been directed to as in for disease the therapy of IL-6 and/or IL-17 inflammatory conditions.Following autoimmunity Disease be suitable for by administration Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or Hydrate, the therapeutical uses of BET suppression are reached because of its remarkable effect to IL-6 and/or IL-17：Acute disseminated brain ridge Marrow inflammation (T.Ishizu et al., " CSF cell factors and chemotactic factor (CF) overview (CSF in acute diseminated encephalomyelitis Cytokine and chemokine profiles in acute disseminated encephalomyelitis) ",《God Through Journal of Immunology (J Neuroimmunol)》175(1-2)：52-8 (2006)), agammaglobulinemia (M.Gonzalez-Serrano et al., " with the patient of X linked agammaglobulinemias carry out lipopolysaccharides stimulation after, Pro-inflammatory cytokine produces increase (Increased Pro-inflammatory Cytokine Production After Lipopolysaccharide Stimulation in Patients with X-linked Agammaglobulinemia) ",《Clinical immunology magazine (J Clin Immuno)》32(5)：967-74 (2012)), allergy Property disease (L.McKinley et al., " the cell-mediated mouse steroid airway inflammations of TH17 and airway hyper-reaction (TH17cells mediate steroid-resistant airway inflammation and airway Hyperresponsiveness in mice) ",《Journal of Immunology》181(6)：4089-97 (2008)), stiff property spondylitis (A.Taylan et al., " assess the axle of t helper cell 17 (the Evaluation of the T helper in stiff property spondylitis 17axis in ankylosing spondylitis) ",《International rheumatology (Rheumatol Int)》32(8)：2511-5 (2012)), (Y.Ito et al., " the white element -6 that is situated between is small in the kidney induced with anti-kidney pompon basement membrane antibody for the anti-TBM ephritis of anti-GBM/ Pathogenetic significance (Pathogenic significance of in the patient of ball ephritis and multinucleate giant cell interleukin-6 in a patient with antiglomerular basement membrane antibody- Induced glomerulonephritis with multinucleated giant cells) ",《US Renal magazine (Am J Kidney Dis)》26(1)：72-9 (1995)), antiphospholipid syndrome (P.Soltesz et al., " with endothelial dysfunction phase Immune characteristic (the Immunological features of primary anti-of the primary anti-phospholipid syndrome of pass Phospholipid syndrome in connection with endothelial dysfunction) ",《Rheumatology》 (Oxford) 47 (11)：1628-34 (2008)), LADA alpastic anemia (Y.Gu et al., it is " poor in aplastic In blood, interleukin (IL) -17 contributes to macrophage to produce IL-8, IL-6 and tumor necrosis factor-alpha (Interleukin (IL) -17promotes macrophages to produce IL-8, IL-6 and tumour necrosis factor- Alpha in aplastic anaemia) ",《Britain's hematology magazine (Br J Haematol)》142(1)：109-14 (2008)), (L.Zhao et al., " interleukin-17 contributes to by inducing the expression of liver interleukin-6 to facilitate oneself immunity hepatitis Morbidity (the Interleukin-17 contributes to the pathogenesis of of oneself immunity hepatitis Autoimmune hepatitis through inducing hepatic interleukin-6 expression) ",《It is public Scientific library synthesis altogether》6(4)：E18909 (2011)), Autoimmune Inner Ear Disease (B.Gloddek et al., " on sense Neural hearing loss is felt, to pharmacological effect (the Pharmacological influence on of inner ear endothelial cell inner ear endothelial cells in relation to the pathogenesis of sensorineural Hearing loss) ",《Otolaryngology is in progress (Adv Otorhinolaryngol)》59: 75-83 (2002)), autoimmunity Property myocarditis (T.Yamashita et al., " IL-6 mediations are broken up to the experimental autoimmune heart by ROR γ t Th17 Most important (the IL-6-mediated Th17 differentiation through RORgammat is of initiation of myositis Essential for the initiation of experimental autoimmune myocarditis ",《It is cardiovascular Study (Cardiovasc Res)》91(4)：640-8 (2011)), autoimmune pancreatitis (J.Ni et al., " interleukin-17 A Participate in injury of pancreas (the Involvement of Interleukin-17A in of Rat Experimental acute necrotic pancreatitis Pancreatic Damage in Rat Experimental Acute Necrotizing Pancreatitis) ",《Inflammation (Inflammation)》(2012)), autoimmune retinopathy (S.Hohki et al. the, " blocking of interleukin-6 signal transduction By suppressing inflammatory Th17 response inhabitations experimented autoimmune myositis (Blockade of interleukin-6 signaling suppresses experimental autoimmune uveoretinitis by The inhibition of inflammatory Th17 responses) ",《(Exp Eye Res) studies in experimental eye section》91 (2)：162-70 (2010)), autoimmune thrombocytopenic purpura (D.Ma et al., " Th17 cell factors (IL-17, TGF-β, IL-6) and Th1 cell factors (IFN-γ) the patient's body with immunologic thrombocytopenic purpura overview (Profile of Th17cytokines (IL-17, TGF-beta, IL-6) and Thl cytokine (IFN-gamma) in Patients with immune thrombocytopenic purpura) ",《Hematology yearbook (Ann Hematol)》87 (11)：899-904 (2008)), Behcet's disease (T.Yoshimura et al., " in Autoimmune uveitis Th17 cells Effect (the Involvement of Th17 cells and the effect of anti-of participation situation and anti-IL-6 therapies IL-6therapy in autoimmune uveitis) ",《Rheumatology》(Oxford) 48 (4)：347-54 (2009)), bleb Property pemphigoid (L.D ' Auria et al., " cell factor and bullous pemphigoid (Cytokines and bullous Pemphigoid) ",《European cytokine network (Eur Cytokine Netw)》10(2)：123-34 (1999)), Ka Sier Graceful disease (H.El-Osta and R.Kurzrock, " castleman's disease：(Castleman ' the s from fundamental mechanism to molecule therapy disease：From basic mechanisms to molecular therapeutics) ",《Oncologist (Oncologist)》16(4)：497-511 (2011)), chylous diarrhea (A.Lahdenpera et al. the, " abdominal disease of untreated In, rather than the up-regulation (Up-regulation of the small intestine interleukin-17 immunity in potential abdominal disease or type 1 diabetes of small intestinal interleukin-17 immunity in untreated coeliac disease but The diabetes of not in potential coeliac disease or in type 1) ",《Clinical trial immunology (Clin Exp Immunol)》167(2)：226-34 (2012)), churg-Strauss syndrome (A.Fujioka et al., " from Qiu-apply Er Shi MRNA expression (the The analysis of mRNA expression of of cutaneous lesions analysis cell factor in syndrome Cytokines from skin lesions in Churg-Strauss syndrome) ",《Dermatology magazine (J Dermatol)》25(3)：171-7 (1998)), Crohn's disease (V.Holtta et al., " IL-23/IL-17 immunity as gram The mark (IL-23/IL-17 immunity as a hallmark of Crohn ' s disease) of engler sieve disease ",《Inflammation Property enteropathy (Inflamm BowelDis)》14(9)：1175-84 (2008)), Ke's radicular syndrome (M.Shibuya et al., " multiple Torr pearl monoclonal antibody successful treatment (Successful treatment with are used in the case of miscellaneous Ke's radicular syndrome and aortitis Tocilizumab in a case of Cogan ' s syndrome complicated with aortitis) ",《Modernism Diseases caused by dampness (Mod Rheumatol)》(2012)), dry eye syndrome (C.De Paiva et al., " and stress it is exhausted after, IL-17 Destroy cornea barrier (IL-17 disrupts corneal barrier following desiccating stress) ", 《Mucosal immunology (Mucosal Immunol)》2(3)：243-53 (2009)), primary mixed type cryoglobulinemia (A.Antonelli et al., " pro-inflammatory cytokine Interleukin -1β, interleukin-6 and tumour in mixed type cryoglobulinemia Serum content (the Serum levels of proinflammatory cytokines interleukin- of necrosin ＆ 1beta, interleukin-6, and tumor necrosis factor alpha in mixed Cryoglobulinemia) ",《A＆R (Arthritis Rheum)》60(12)：3841-7 (2009)), musculus cutaneus It is scorching that (G.Chevrel et al., " interleukin-17 adds influences of the IL-1 β to myocyte：T cell acts in myositis pathogenesis Argument (Interleukin-17 increases the effects of IL-1beta on muscle cells： Arguments for the role of T cells in the pathogenesis of myositis) ",《Nerve immunity Learn magazine》137(1-2)：125-33 (2003)), devic's disease (U.Linhares et al., " produced in vitro by CD4 (+) T cell Life IL-6 and IL-21 (The Ex Vivo Production of directly relevant with the nerve loss in neuromyelitis optica patient IL-6 and IL-21 by CD4(+)T Cells is Directly Associated with Neurological Disability in Neuromyelitis Optica Patients) ",《Clinical immunology magazine》(2012)), encephalitis (D.Kyburz and M.Corr, " in the case where lacking TGF-β, caused Th17 cells are based on the experimental mistake of adoptive transfer induction Quick property encephalitis (Th17 cells generated in the absence of TGF-beta induce experimental Allergic encephalitis upon adoptive transfer) ",《Clinical immunology expert summarizes (Expert Rev Clin Immunol)》7(3)：283-5 (2011)), eosinophilic esophagitis (P.Dias and G.Banerjee, " Th17/IL-17 pairs The effect (The Role of Th17/IL-17 on Eosinophilic Inflammation) of Eosinophilic Inflammation ", 《Autoimmunity magazine (J Autoimmun)》(2012)), eosinophilic fasciitis (P.Dias and G.Banerjee,《It is autologous to exempt from Epidemic disease power magazine》(2012)), erythema nodosum (I.Kahawita and D.Lockwood, " to the pathology of leprosy erythema nodosum Understanding (Towards understanding the pathology of erythema nodosum leprosum) ",《Emperor Family's tropical medicine can be reported (Trans R Soc Trop Med Hyg) with Society of Public Health》102(4)：329-37 (2008)), it is big and small Born of the same parents' arteritis (J.Deng et al., " Th17 and Th1 t cell responses (the Th17 and Th1 T-cell in giant cell arteritis Responses in giant cell arteritis) ",《Circulation》121(7)：906-15 (2010)), glomerulonephritis (J.Ooi et al., " summary：T aids in 17 cells：Its effect (Review in glomerulonephritis：T helper 17 cells：Their role in glomerulonephritis) ",《Nephrology (Nephrology)》(Carlton (Carlton))15(5)：513-21 (2010)), goodpasture's syndrome (Goodpasture ' s syndrome) (Y.Ito Et al., " interleukin-6 is in the glomerulonephritis induced with anti-kidney pompon basement membrane antibody and the patient of multinucleate giant cell Pathogenetic significance ",《US Renal magazine》26(1)：72-9 (1995)), granulomatous Polyangiitis (Wegener) (H.Nakahama et al., " treatment of interleukin-6 and other laboratory parameters to the patient with Wei Genashi granulomas disease Uniqueness reaction (Distinct responses of interleukin-6 and other laboratory parameters To treatment in a patient with Wegener ' s granulomatosis) ",《Internal medicine (Intern Med)》 32(2)：189-92 (1993)), Graves disease (S.Kim et al., " serum interleukin-17 in graves' ophthalmopathy increase (Increased serum interleukin-17 in Graves ' ophthalmopathy) ",《Robert Graves clinic with Test ophthalmology (Graefes Arch Clin Exp Ophthalmol)》250(10)：1521-6 (2012)), Ji Lan-Ba Lei Syndrome (M.Lu and J.Zhu, " effect (The role of cytokines of the cell factor in Guillain-Barre＆1＆ syndrome In Guillain-Barre syndrome) ",《Neurology magazine (J Neurol)》258(4)：533-48 (2011)), bridge Ben's thyroiditis (N.Figueroa-Vega et al., " circulates pro-inflammatory cytokine and Th17 leaching in Hashimoto's thyroiditis Bar cell increase (Increased circulating pro-inflammatory cytokines and Th17 Lymphocytes in Hashimoto ' s thyroiditis) ",《Clinical endocrinology and metabolic magazine (J Clin Endocrinol Metab)》95(2)：953-62 (2009)), (L.Xu et al., " Th17 cells are in autoimmunity for hemolytic anemia Developing key effect (the Critical role of Th17 cells in development of of property hemolytic anemia Autoimmune hemolytic anemia) ",《Experimental hematology (Exp Hematol)》(2012)), purpura,Henoch-Schonlein (H.Jen et al., " serum interleukin-17 and the increase of tip Th17 cells in the children with acute purpura,Henoch-Schonlein (Increased serum interleukin-17 and peripheral Th17 cells in children with Acute Henoch-Schonlein purpura) ",《Children's allergy and immunology (Pediatr Allergy Immunol)》 22(8)：862-8 (2011)), IgA nephrosis (F.Lin et al. the, " imbalance of regulatory T-cell and Th17 cells in IgA nephrosis (Imbalance of regulatory T cells to Th17 cells in IgA nephropathy) ",《What this was born receives Tie up subclinical laboratory investigation magazine (Scand J Clin Lab Invest)》72(3)：221-9 (2012)), inclusion body myositis (P.Baron et al., " mankind sarcoblast stimulated by using A β produces IL-6：Correlation in IBM pathogenesis (Production of IL-6 by human myoblasts stimulated with Abeta：relevance in the Pathogenesis of IBM) ",《Neurology (Neurology)》57(9)：1561-5 (2001)), type i diabetes (A.Belkina and G.Denis,《Natural cancer summary》12(7)：465-77 (2012)), interstitial cystitis (L.Lamale Et al., " interleukin-6, histamine and methylhistamine as interstitial cystitis diagnostic marker (Interleukin-6, Histamine, and methylhistamine as diagnostic markers for interstitial Cystitis) ",《Urology (Urology)》68(4)：702-6 (2006)), Kawasaki disease (S.Jia et al., " patients with Kawasaki disease body The interior regulatory T-cell of T auxiliary types 17/ imbalance (The T helper type 17/regulatory T cell Imbalance in patients with acute Kawasaki disease) ",《Clinical trial immunology》162(1)： 131-7 (2010)), leukocytoclastic angiitis (Min, C.K. et al., " in patients with malignant myeloma after bortezomib therapy Skin leukocytoclastic angiitis (LV)；With correlation (the Cutaneous leucoclastic of pro-inflammatory cytokine vasculitis(LV)following bortezomib therapy in a myeloma patient；association With pro-inflammatory cytokines) ",《European haematol magazine (Eur J Haematol)》76(3)： 265-8 (2006)), lichen planus (N.Rhodus et al., " before with dexamethasone in treatment (aggressivity) oral lichen planus Pro-inflammatory cytokine content in saliva (Proinflammatory cytokine levels in saliva afterwards before and after treatment of(erosive)oral lichen planus with Dexamethasone) ",《Mouth disease (Oral Dis)》12(2)：112-6 (2006)), lupus (SLE) (M.Mok et al., " interleukin-17 (IL-17) and IL-23 and Th1/Th2 cell factors and the relation of Disease Activity in systemic lupus erythematosus (The relation of interleukin 17(IL-17)and IL-23to Th1/Th2cytokines and Disease activity in systemic lupus erythematosus) ",《Rheumatology magazine (J Rheumatol)》37(10)：2046-52 (2010)), microscopic polyangitis (A.Muller Kobold et al., " in Wei lattice The external upper endothelium that reconciles for the E-Selectin realized in Na Shi granulomas disease and microscopic polyangitis by autoantibody is thin Induction (the In vitro up-regulation of E-selectin and induction of of interleukin-6 in born of the same parents interleukin-6 in endothelial cells by autoantibodies in Wegener′s Granulomatosis and microscopic polyangiitis) ",《Clinical and experiment rheumatology (Clin Exp Rheumatol)》17(4)：433-40 (1999)), multiple sclerosis (F.Jadidi-Niaragh and A.Mirshafiey, " Th17 cells：New player (Th17 cell, the new player of of neuroinflammatory process in multiple sclerosis Neuroinflammatory process in multiple sclerosis) ",《Scandinavia Journal of Immunology (Scand J Immunol)》74(1)：1-13 (2011)), myasthenia gravis (R.Aricha et al., " block IL-6 Inhibition tests Property LADA myasthenia gravis (Blocking of IL-6 suppresses experimental autoimmune Myasthenia gravis) ",《Autoimmunity magazine》36(2)：135-41 (2011)), myositis (G.Chevrel et al., " interleukin-17 adds influences of the IL-1 β to myocyte：The argument that T cell acts in myositis pathogenesis (Interleukin-17 increases the effects of IL-1 beta on muscle cells：arguments For the role of T cells in the pathogenesis of myositis) ",《Neuroimmunology magazine》137 (1-2)：125-33 (2003)), optic neuritis (S.Icoz et al., " aquaporin protein-4 antibody positive neuromyelitis optica suffer from IL-6 produces enhancing (Enhanced IL-6 production in aquaporin-4 antibody positive in person Neuromyelitis optica patients) ",《International Journal of Neuroscience (Int J Neurosci)》120(1)：71-5 (2010)), (E.Lopez-Robles et al., " TNF α and IL-6 are the amboceptors in the bubbling process of pemphigus to pemphigus (TNFalpha and IL-6 are mediators in the blistering process of pemphigus) ",《State Border dermatology magazine (Int J Dermatol)》40(3)：185-8 (2001)), POEMS syndromes (K.Kallen et al., " IL-6 relies on the new development in sexual biology and therapy：It is what that we, which are in which kind of position and opinion,(New developments in IL-6dependent biology and therapy：where do we stand and what are the options)”《Investigational agent expert opinion (Expert Opin Investig Drugs)》8(9)：1327-49 (1999)), PAN (T.Kawakami et al. the, " blood of cutaneous polyarteritis nodosa patient's body interleukin-6 Clear content (Serum levels of interleukin-6 in patients with cutaneous polyarteritis Nodosa) ",《Dermatology journal (Acta Derm Venereol)》92(3)：322-3 (2012)), primary biliary liver (K.Harada et al., " conduit week interleukin-17 generation joint bile innate immunity facilitates primary biliary for hardening Pathogenesis (the Periductal interleukin-17production in association of cholepathia in hepatic sclerosis with biliary innate immunity contributes to the pathogenesis of Cholangiopathy in primary biliary cirrhosis) ",《Clinical trial immunology》157(2)：261-70 (2009)), (S.Fujishima et al., " IL-17F is participated in psoriasis psoriasis by inducing IL-6 (Involvement of IL-17F via the induction of IL-6in psoriasis) ",《Skin disorder is related Archial research (Arch DermatolRes)》302(7)：499-505 (2010)), arthritic psoriasis (S.Raychaudhuri et al., IL-17 acceptor and its functional meaning (IL-17 receptor in arthritic psoriasis And its functional significance in psoriatic arthritis) ",《Molecule and cellular biochemistry (Mol Cell Biochem)》359(1-2)：419-29 (2012)), pyoderma gangraenosum (T.Kawakami et al., " pass through grain Cell and monocyte adsorbing separation reduce pyoderma gangraenosum and interleukin-6, Bai Jie in patients of ulcerative colitis body Element -8 and anti-phosphatidylserine-factor compound antibody (Reduction of interleukin-6, interleukin- 8, and anti-phosphatidylserine-prothrombin complex antibody by granulocyte and monocyte adsorption apheresis in a patient with pyoderma gangrenosum and Ulcerative colitis) ",《American journal of gastroenterology (Am J Gastroenterol)》104(9)：2363-4 (2009)), (M.Kawai et al., " two intractable relapsing polychondritis patient's bodies are for anti-white for relapsing polychondritis Lasting reaction (Sustained response the to tocilizumab, anti-of the receptor antibody Torr pearl monoclonal antibody of interleukin -6 Interleukin-6receptor antibody, in two patients with refractory relapsing Polychondritis) ",《Rheumatology》(Oxford) 48 (3)：318-9 (2009)), rheumatoid arthritis (Z.Ash and P.Emery, " effect (The role of tocilizumab in the of the Torr pearl monoclonal antibody in rheumatoid arthritis is managed Management of rheumatoid arthritis) ",《Biotherapy expert opinion (Expert Opin Biol Ther)》, 12 (9)：1277-89 (2012)), sarcoidosis (F.Belli et al., " diagnose and be classified Granuloma in lung disease Cytokine analysis (Cytokines assay in peripheral in middle peripheral blood and bronchoalveolar lavage blood and bronchoalveolar lavage in the diagnosis and staging of pulmonary Granulomatous diseases) ",《International immunopathology and pharmacology magazine (Int J Immunopathol Pharmacol)》13(2)：61-67 (2000)), chorionitis (T.Radstake et al., " in Systemic sclerosis (SSc) significantly Th17 overviews and the cell inner expression of TGF β and IFN γ distinguish SSc phenotypes (The pronounced Th17 profile in systemic sclerosis(SSc)together with intracellular expression of TGFbeta and IFNgamma distinguishes SSc phenotypes) ",《Public science library integrates》, 4 (6)：E5903 (2009)), Sjogren syndrome (G.Katsifis et al., it is " relevant with qualified human relations syndrome immunopathogenesis Systemic and local interleukin-17 and relevant cell factor (Systemic and local interleukin-17 and Linked cytokines associated with Sjogren ' s syndrome immunopathogenesis) ",《It is beautiful State's pathology magazine》175(3)：1167-77 (2009)), (Y.Sun et al., " MMP-9 and IL-6 are Gao Andong to takayasu's arteritis Potential source biomolecule mark (the MMP-9 and IL-6are potential biomarkers for of Disease Activity in arteries and veins inflammation Disease activity in Takayasu ' s arteritis) ",《International Cardiology magazine (Int J Cardiol)》 156(2)：236-8 (2012)), transverse myelitis (J.Graber et al., " in transverse myelitis and multiple sclerosis Interleukin-17 (Interleukin-17 in transverse myelitis and multiple sclerosis) "《God Through Journal of Immunology》196(1-2)：124-32 (2008)), ulcerative colitis (J.Mudter and M.Neurath, it is " inflammatory I1-6 signal transductions in enteropathy：Pathological Physiology acts on and clinical correlation (Il-6signaling in inflammatory bowel disease：Pathophysiological role and clinical relevance) ",《IBD》13 (8)：1016-23 (2007)), uveitis (H.Haruta et al., " block interleukin-6 signal transduction not only inhibit thl 7, and by promoting the regulatory T-cell in experimented autoimmune myositis, it is suppressed that class regards between light receptor Flavine associated proteins specificity T h1 (Blockade of interleukin-6signaling suppresses not only th17 but also interphotoreceptor retinoid binding protein-specific Th1 by Promoting regulatory T cells in experimental autoimmune uveoretinitis) ",《Ophthalmology Research and eyesight (Invest Ophthalmol Vis Sci)》52(6)：3264-71 (2011)) and leucoderma (D.Bassiouny and O.Shaker, " effect (Role of of the interleukin-17 in the pathogenesis of leucoderma Interleukin-17 in the pathogenesis of vitiligo) ",《Clinical and experimental dermatology (Clin Exp Dermatol)》36(3)：292-7 115.(2011)).Therefore, the present invention includes Formulas I and Formula II compound, its alloisomerism Body, dynamic isomer, pharmaceutically acceptable salt or hydrate；Drug regimen comprising one or more of those compounds Thing；And the method that these diseases are treated using those compounds or composition.

Acute and chronic (non-self immunity) diseases associated with inflammation characterized by the expression increase of pro-inflammatory cytokine It is also suitable for therapeutic BET to suppress, pro-inflammatory cytokine includes IL-6, MCP-1 and IL-17.These diseases include (but unlimited In) (D.Bradley and S.Kountakis, " be situated between white element and transforming growth factor β are in chronic nasosinusitis and nasal polyposis for nasosinusitis In effect (Role of interleukins and transforming growth factor-beta in chronic Rhinosinusitis and nasal polyposis) ",《Laryngoscope (Laryngoscope)》115(4)：684-6(2005))、 Pneumonia (Besnard, A.G. et al. the, " inflammatory body-IL-1-Th17 reactions (Inflammasome-IL-1- in hylactic pneumonia Th17 response in allergic lung inflammation)”《Molecular cytobiology magazine (J Mol Cell Biol)》4(1)：3-10 (2012)), osteomyelitis (T.Yoshii et al., " because aurococcus caused by muroid Interleukin -1β in osteomyelitis experimental model, interleukin-4, the local content (Local of interleukin-6 and tumor necrosis factor α Levels of interleukin-1beta, -4, -6 and tumor necrosis factor alpha in an Experimental model of murine osteomyelitis due to staphylococcus aureus) ",《Carefully Intracellular cytokine (Cytokine)》19(2)：59-65 2002)), gastritis (T.Bayraktaroglu et al., " with pylorus spiral In the dyspeptic patient of the related gastritis of bacillus, the serum content of tumor necrosis factor-alpha, interleukin-6 and interleukin-8 Do not increase (Serum levels of tumor necrosis factor-alpha, interleukin-6 and interleukin-8 are not increased in dyspeptic patients with Helicobacter Pylori-associated gastritis) ",《Mediator of inflammation (Mediators Inflamm)》13(1)：25-8(2004))、 Enteritis (K.Mitsuyama et al., " facilitates returning in SAMP1/Yit mouse by across the signal transduction activation STAT3 of interleukin 6 Enteritis (STAT3activation via interleukin 6trans-signalling contributes to ileitis In SAMP1/Yit mice) ",《Enteron aisle (Gut)》55(9)：1263-9. (2006)), gingivitis (R.Johnson et al., it is " white The pathogenesis of interleukin -11 and IL-17 and periodontosis (Interleukin-11and IL-17 and the Pathogenesis of periodontal disease) ",《Periodontology (JPeriodontol)》75(1)：37-43 (2004)), appendicitis (S.Latifi et al., " and in abdomen in septicemia serum IL-6 persistently raise differentiate the hospital stays compared with Those long (Persistent elevation of serum interleukin-6 in intraabdominal sepsis Identifies those with prolonged length of stay) ",《Pediatric surgery magazine (JPediatr Surg)》39(10)：1548-52 (2004)), irritable colon syndrome (M.Ortiz-Lucas et al., " irritable colon syndrome It is immune to assume Part II：Effect (the Irritable bowel syndrome immune of cell factor hypothesis.Part two：The role of cytokines) ",《Gastroenterology comments on (Rev Esp Enferm Dig)》102(12)：711-7 (2010)), tissue transplantation rejection reaction (L.Kappel et al., " and IL-17 facilitate CD4 mediate shifting Plant versus-host disease (IL-17 contributes to CD4-mediated graft-versus-host disease) ", 《Blood》113(4)：945-52 (2009)), chronic obstructive pulmonary disease (COPD) (S.Traves and L.Donnelly, " air flue disease Th17 cells (Th17 cells in airway diseases) in disease ",《Current molecular medicine (Curr Mol Med)》8 (5)：416-26 (2008)), septic shock (toxic shock syndrome, TSS, SIRS, bacterium septicemia etc.) (E.Nicodeme etc. People,《It is natural》468(7327)：1119-23 (2010)), osteoarthritis (L.Chen et al., " in muroid osteoarthritis, Mediation that IL-17RA is fit, which suppresses IL-6, can suppress synovial membrane inflammation (IL-17RA aptamer-mediated repression of IL-6 inhibits synovium inflammation in a murine model of osteoarthritis)”.《Bone Arthritis and cartilage (Osteoarthritis Cartilage)》19(6)：711-8 (2011)), acute gout (W.Urano etc. People, " during acute gouty arthritis, the inflammatory processes (The in serum uric acid concentration reduction mechanism inflammatory process in the mechanism of decreased serum uric acid Concentrations during acute gouty arthritis) ",《Rheumatology magazine》29(9)：1950-3 (2002)), ALI (S.Traves and L.Donnelly, " the Th17 cells in airway disorders ",《Current molecular medicine》 8(5)：416-26 (2008)), acute renal failure (E.Simmons et al., " plasma levels of cytokines content prediction acute renal failure suffer from The death rate (the Plasma cytokine levels predict mortality in patients with acute of person Renal failure) ",《International Nephrology (Kidney Int)》65(4)：1357-65 (2004)), burn (P.Paquet and G.Pierard, " interleukin-6 and skin (Interleukin-6 and the skin) ",《International allergy and immunology archives (Int Arch Allergy Immunol)》109(4)：308-17 (1996)), herxheimer reaction (G.Kaplanski et al., " it is refined- Conspicuous Er Shi reactions make the hot endocarditic treatments of chronic Q complicate：Elevated TNF α and IL-6 serum content (Jarisch- Herxheimer reaction complicating the treatment of chronic Q fever endocarditis：Elevated TNFalpha and IL-6serum levels) ",《Infectious disease magazine (J Infect)》 37(1)：83-4 (1998) and the SIRS relevant with viral infection (A.Belkina and G.Denis,《Natural cancer summary》 12(7)：465-77(2012)).Therefore, the present invention includes Formulas I and Formula II compound, its stereoisomer, dynamic isomer, medicine Acceptable salt and hydrate on；Pharmaceutical composition comprising one or more of those compounds；And use that A little compounds or composition treat the method for these diseases.

In one embodiment, BET inhibitor Formulas I or Formula II compound or its stereoisomer, mutually variation can be used Structure body, pharmaceutically acceptable salt or hydrate or composition comprising one or more of those compounds treat class Rheumatic arthritis (RA) and multiple sclerosis (MS).On effectiveness of the BET inhibitor in RA and MS preclinical models, Strong proprietary data be present.R.Jahagirdar et al., " in mouse multiple sclerosis model, oral biology is available Small molecule RVX-297 significantly reduce disease ",《World's inflammation meeting》, Paris, FRA (2011).RA and MS feature is all IL-6 and IL-17 inflammation sexual approach dysregulations (A.Kimura and T.Kishimoto, " IL-6：The regulation of Treg/Th17 balances The factor ",《European Journal of Immunology》40(7)：1830-5 (2010)) and therefore will suppress particularly sensitive to BET.At another In embodiment, BET inhibitor Formulas I or Formula II compound or its stereoisomer, dynamic isomer can be used, pharmaceutically may be used The salt or hydrate of receiving or the composition comprising one or more of those compounds treat septicemia and related diseases Bitterly.Published data (E.Nicodeme et al.,《It is natural》468(7327)：1119-23 (2010)) and proprietary data in, BET Suppress display, in preclinical models, partly suppress the development of septicemia by suppressing IL-6 expression.

In one embodiment, BET inhibitor Formulas I or Formula II compound or its stereoisomer, mutually variation can be used Structure body, pharmaceutically acceptable salt or hydrate or composition comprising one or more of those compounds treat cancer Disease.Cancer pair with overexpression, transposition, amplification or restructuring c-myc or other myc family tumors albumen (MYCN, L-myc) BET suppresses particularly sensitive.J.Delmore et al.,《Cell》146(6)：904-17(2010)；J.Mertz et al.,《American National Academy of sciences's proceeding》108(40)：16669-74(2011).These cancers include but is not limited to the white blood of acute lymphoblastic B Disease, Burkitt's lymphoma, diffusivity large celllymphoma, Huppert's disease, primary plasma cell leukemia, atypia class Cancer lung cancer, carcinoma of urinary bladder, breast cancer, cervical carcinoma, colon cancer, stomach cancer, spongioblastoma, hepatocellular carcinoma, interior point of maxicell nerve Secrete cancer, medulloblastoma, nodular melanoma, superficial spreading melanoma, neuroblastoma, esophageal squamous cell Cancer, osteosarcoma, oophoroma, prostate cancer, clear cell carcinoma of kidney, retinoblastoma, rhabdomyosarcoma and cellule lung Cancer.M.Vita and M.Henriksson,《Carcinobiology seminar (Semin Cancer Biol)》16(4)：318-30 (2006)。

In one embodiment, BET inhibitor Formulas I or Formula II compound or its stereoisomer, mutually variation can be used Structure body, pharmaceutically acceptable salt or hydrate or composition comprising one or more of those compounds come treat by Cancer caused by the abnormal regulation (overexpression, transposition etc.) of BET protein.These cancers include but is not limited to NUT center line cancers (Brd3 or Brd4 translocate to the genes of nutlin 1) (C.French《Cancer genet and cytogenetics (Cancer Genet Cytogenet)》203(1)：16-20 (2010)), B cell lymphoma (Brd2 overexpressions) (R.Greenwald et al.,《Blood》 103(4)：1475-84 (2004)), non-small cell lung cancer (BrdT overexpressions) (C.Grunwald et al., " in non-small cell lung cancer After multiple into regulation cancer/germ line gene expression (Expression of multiple epigenetically Regulated cancer/germline genes in nonsmall cell lung cancer) ",《International journal of cancer》 118(10)：2522-8 (2006)), the cancer of the esophagus and head and neck squamous cell carcinoma (BrdT overexpressions) (M.Scanlan et al., " lung The expression of cancer-testis antigen in cancer：Bromine domain testicle specificity gene (BRDT) is defined as new CT gene Cs T9 (Expression of cancer-testis antigens in lung cancer：definition of Bromodomain testis-specific gene (BRDT) as a new CT gene, CT9) ",《Cancer communicates (Cancer Lett)》150(2)：55-64 (2000)) and colon cancer (Brd4) (R.Rodriguez et al., " bromine structure in Human colon cancer Domain BRD4 abnormal epigenetic regulation (Aberrant epigenetic regulation of bromodomain BRD4in Human colon cancer) ",《Molecular medicine magazine (J Mol Med)》(Berlin) 90 (5)：587-95(2012)).

In one embodiment, because BET inhibitor reduces pTEFb and the Brd for participating in the gene of cell propagation is relied on Property raise, it is possible to use BET inhibitor Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically Acceptable salt or hydrate or composition comprising one or more of those compounds are treated dependent on pTEFb (Cdk9/ cyclin T) and BET protein adjust the cancer of oncogene.These cancers are including but not limited to chronic (W.Tong et al., " the inhibitor SNS-032 of potent selective Cdk2,7 and 9 exists for lymphocytic leukemia and Huppert's disease I phases and drug research (Phase I and in patient with advanced chronic lymphocytic leukemia and Huppert's disease Pharmacologic study of SNS-032, a potent and selective Cdk2,7, and 9inhibitor, in patients with advanced chronic 1ymphocytic leukemia and multiple Myeloma) ",《Journal of Clinical Oncology (J Clin Oncol)》28(18)：3015-22 (2010)), follicular lymphoma, tool There are the diffusivity large B cell lymphoid tumor of centrum germinativum's phenotype, Burkitt's lymphoma, hodgkin's lymphomas, follicularis leaching Bar knurl and the primary cutaneous type of activation (C.Bellan et al., " during normal lymphoid differentiation and vicious transformation CDK9/ Cyclin T1s express (CDK9/CYCLIN T1 expression during normal lymphoid Differentiation and malignant transformation) ",《Pathology magazine (J Pathol)》203(4)： 946-52 (2004)), neuroblastoma and primary nervous ectoderm tumour (G.De Falco et al., " Cdk9 regulation nerves Break up and it expresses (Cdk9 regulates neural related to the differentiation rank of neuroblastoma and PNET tumours differentiation and its expression correlates with the differentiation grade Of neuroblastoma and PNET tumors) ",《Carcinobiology and therapy (Cancer Biol Ther)》4(3)： 277-81 (2005)), rhabdomyosarcoma (C.Simone and A.Giordano, " abolish mankind's RD human rhabdomyosarcoma cells in Signal dependence activation (the Abrogation of signal-dependent of cdk9/ cyclin T2 a compounds activation of the cdk9/cyclin T2a complex in human RD rhabdomyosarcoma Cells) ",《Cell death and differentiation (Cell Death Differ)》14(1)：192-5 (2007)), prostate cancer (D.Lee Et al., " androgen receptor and positive elongation factors P-TEFb interact and improve the efficiency (Androgen of transcription extension receptor interacts with the positive elongation factor P-TEFb and enhances The efficiency of transcriptional elongation) ",《Journal of biological chemistry》276(13)：9978-84 (2001)) and breast cancer (K.Bartho1omeeusen et al., " and BET bromines domain suppress by of short duration from 7SK snRNP Property release P-TEFb activated transcriptions (BET bromodomain inhibition activates transcription via a Transient release of P-TEFb from 7SK snRNP) ",《Journal of biological chemistry》(2012)).

In one embodiment, BET inhibitor Formulas I or Formula II compound or its stereoisomer, mutually variation can be used Structure body, pharmaceutically acceptable salt or hydrate or composition comprising one or more of those compounds are treated such as The cancer of the BET such as CDK6, Bcl2, TYRO3, MYB and hTERT response genes up-regulation.M.Dawson et al.,《It is natural》478 (7370)：529-33(2011)：J.Delmore et al.,《Cell》146(6)：904-17(2010).These cancers are included (but not Be limited to) cancer of pancreas, breast cancer, colon cancer, spongioblastoma, adenoid cystic carcinoma, T cell pre-lymphocytic leukemia, dislike Nerve glioma, carcinoma of urinary bladder, medulloblastoma, thyroid cancer, melanoma, Huppert's disease, Barrett gland cancer (Barret ' s adenocarcinoma), hepatoma, prostate cancer, promyelocytic leukemia, chronic lymphocytic are white Blood disease, lymphoma mantle cell, diffusivity large B cell lymphoid tumor, ED-SCLC and kidney.M.Ruden and N.Puri, " target To the novel anti-cancer therapy (Novel anticancer therapeutics targeting telomerase) of Telomerase ", 《Treatment of cancer is summarized》(2012)；P.Kelly and A.Strasser, " Bcl-2 and its rush relatives living treat in tumorigenicity and cancer Effect (The role of Bcl-2and its pro-survival relatives in tumourigenesis in method and cancer therapy)”《Cell death and differentiation》18(9)：1414-24(2011)；T.Uchida et al., " bcl-2 is anti- Antitumor action (Antitumor of the adopted oligodeoxynucleoside phosphorothioate to external mankind kidney cell's cancer cell and in mouse effect of bcl-2 antisense phosphorothioate oligodeoxynucleotides on human Renal-cell carcinoma cells in vitro and in mice) ",《Molecule urology (Mol Urol)》5(2)： 71-8(2001)。

Published data and proprietary data show that BET suppresses to directly affect to what the cell in various cancers was bred. In one embodiment, BET inhibitor Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmacy can be used Upper acceptable salt or hydrate or composition comprising one or more of those compounds treat following cancer, pin To the cancer, published data be present, and for certain cancers, exist inside proprietary and/or vitro data, these numbers According to showing that BET suppresses cell proliferation and directly affect.These cancers include NMC (NUT center line cancers), the white blood of acute myeloid Sick (AML), acute B lymphoblastic leukemia (B-ALL), Burkitt's lymphoma, B cell lymphoma, melanoma, mixing It is leukaemia, Huppert's disease, promyelocytic leukemia (PML) and non Hodgkin lymphom. P.Filippakopoulos et al.,《It is natural》468(7327)：1067-73(2010)；M.Dawson et al.,《It is natural》478 (7370)：529-33(2011)；Zuber, J. et al., " RNAi screenings differentiate Brd4 to be controlling in acute myelogenous leukemia Treat target spot (RNAi screen identifies Brd4as a therapeutic target in acute myeloid Leukaemia) ",《It is natural》478(7370)：524-8(2011)；M.Segura et al.,《Cancer research》72(8)：Supplementary issue 1 (2012).The compounds of this invention has proven to the effect that BET suppresses to breed the cell in vitro of following cancer：Neuroblastoma, Medulloblastoma, lung cancer (NSCLC, SCLC) and colon cancer.

In one embodiment, because potential cooperative effect or cumulative effect between BET inhibitor and other cancer therapies Should, thus BET inhibitor Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or Hydrate or composition comprising one or more of those compounds can be with other therapies, chemotherapeutant or anti-increasings Grow agent combined therapy human cancer and other proliferative disorders.The therapeutic agent that can be combined in treatment of cancer with BET inhibitor Inventory includes but is not limited to ABT-737, azacitidine ((Vidaza) is pricked in Victor), AZD1152 (Barasertibs (Barasertib)), AZD2281 (olaparib (Olaparib)), AZD6244 (department U.S. replaces Buddhist nun (Selumetinib)), It is BEZ235, bleomycin sulfate (Bleomycin Sulfate), bortezomib (Bortezomib) (Bortezomib (Velcade)), white The peace that disappears (Busulfan) (bridle orchid (Myleran)), camptothecine, cis-platinum, endoxan (carat sweet smell (Clafen)), CYT387, Cytarabine (Ara-C), Dacarbazine (Dacarbazine), DAPT (GSI-IX), Decitabine (Decitabine), fill in Meter Song (Dexamethasone), adriamycin (Doxorubicin) (A Deli mycins (Adriamycin)), Etoposide (Etoposide), everolimus (Everolimus) (RAD001), Flavopiridol (Flavopiridol) (Avobenzene west ground (Alvocidib)), Jia Litepi (Ganetespib) (STA-9090), Gefitinib (Gefitinib) (Iressa (Iressa)), idarubicin (Idarubicin), ifosfamide (rice support celestial being (Mitoxana)), IFNa2a (Recomvinated Interferon α-2a A (Roferon A)), melphalan (Melphalan) (L-Sarcolysinum (Alkeran)), plum plug azoles Lars lead to (Methazolastone) (Temozolomide (temozolomide)), melbine (Metformin), mitoxantrone (Mitoxantrone) (Novantrone (Novantrone)), taxol (Paclitaxel), insoral (Phenformin), PKC412 (midostaurins (Midostaurin)), PLX4032 (Wei Luofeini (Vemurafenib)), pomalidomide (Pomalidomide) (CC- 4047), metacortandracin (Prednisone) (delta pine (Deltasone)), rapamycin (Rapamycin), Revlimid (Revlimid) (lenalidomide (Lenalidomide)), Luso profit are for Buddhist nun (Ruxolitinib) (INCB018424), Suo Lafei Buddhist nun (Sorafenib) (Nexavar (Nexavar)), SU11248 (Sutent (Sunitinib)), SU11274, vincaleukoblastinum (Vinblastine), vincristine (Vincristine) (Vincristinum Sulfate (Oncovin)), vinorelbine (Vinorelbine) (promise Wei Ben (Navelbine)), Vorinostat (Vorinostat) (SAHA) and WP1130 (wearing lattice Racine (Degrasyn)).

In one embodiment, BET inhibitor Formulas I or Formula II compound or its stereoisomer, mutually variation can be used Structure body, pharmaceutically acceptable salt or hydrate or composition treatment comprising one or more of those compounds are benign Hypertrophic and fibrotic conditions, including benign soft tissue neoplasm, bone tumour, brain and tumor of spinal cord, eyelid and orbital tumor, granulation It is swollen, lipoma, meningioma, Multiple Endocrine neoplasia, nasal polyp, pituitary tumor, prolactinoma, pseudotumor cerebri, seborrheica Keratosis, polyp of stomach, thyroid nodule, pancreas capsule anything superfluous or useless, hemangioma, vocal nodule, polyp and tumour, castleman's disease, Chronic pilonidal disease, histiocytoma, pilar cyst, pyogenic granuloma, juvenile polyposis syndrome, idiopathic lung fiber Change, kidney fibrosis, postoperative stenosis, keloid formation, chorionitis and cardiac fibrosis.X.Tang et al.,《U.S.'s pathology Magazine》In printing (in press) (2013).

In one embodiment, BET inhibitor Formulas I or Formula II compound or its stereoisomer, dynamic isomer, medicine Acceptable salt or hydrate or the composition comprising one or more of those compounds raise ApoA-1 because of it on The ability of transcription and protein expression (O.Mirguet et al.,《Bioorganic Chemistry communicates with medical chemistry》22(8)：2963-7 (2012)；C.Chung et al.,《Pharmaceutical chemistry magazine》54(11)：3827-38 (2011)), it is possible to for treating generally Related angiocardiopathy, including dyslipidemia, atherosclerosis, hypercholesterolemia and metabolic syndrome (A.Belkina And G.Denis,《Natural cancer summary》12(7)：465-77(2012)；G.Denis《It was found that medicine (Discov Med)》10 (55)：489-99(2010)).In another embodiment, BET inhibitor Formulas I or Formula II compound or its stereoisomer, Dynamic isomer, pharmaceutically acceptable salt or hydrate or composition comprising one or more of those compounds can By for treating the non-cardiovascular disease characterized by ApoA-1 defects, including Alzheimer disease.D.Elliott et al.,《Face Bed blood fat》51(4)：555-573(2010).

In one embodiment, BET inhibitor Formulas I or Formula II compound or its stereoisomer, dynamic isomer, medicine Acceptable salt or hydrate or the composition comprising one or more of those compounds can be used for pancreas islet on The patient of plain resistance and type ii diabetes.A.Belkina and G.Denis,《Natural cancer summary》12(7)：465-77 (2012)；G.Denis《It was found that medicine》10(55)：489-99(2010)；F.Wang et al.,《Journal of biological chemistry》425(1)： 71-83(2010)；G.Denis et al.,《Federation of European biochemistry association bulletin (FEBS Lett)》584(15)：3260-8 (2010).The antiinflammation that BET suppresses is by with the extra value for reducing the inflammation relevant with diabetes and metabolic disease. K.Alexandraki et al. the, " inflammatory processes in diabetes B：Effect (the Inflammatory of cell factor process in type 2diabetes：The role of cytokines) ",《NYAS's yearbook (Ann N YAcad Sci)》1084：89-117(2006).

In one embodiment, BET inhibitor Formulas I or Formula II compound or its stereoisomer, dynamic isomer, medicine Acceptable salt or hydrate or the composition comprising one or more of those compounds open because it lowers virus on The ability of mover, it is possible to which the therapy as the cancer relevant with virus, virus include Epstein-Barr virus (EBV), hepatitis Viral (HBV, HCV), kaposi sarcoma associated herpes virus (Kaposi ' s sarcoma associated virus；KSHV), the mankind Papillomavirus (HPV), Merkel cell polyomavirus (Merkel cell polyomavirus) and human macrophage cell disease Malicious (CMV).D.Gagnon et al.,《Journal of Virology》83(9)：4127-39(2009)；J.You et al.,《Journal of Virology》80 (18)：8909-19(2006)；R.Palermo et al., " rna plymerase ii, which is stagnated, promotes nucleosome occlusion and pTEFb recruitments Immortalized with being driven by Epstein-Barr virus ",《Public science library pathogen》7(10)：e1002334(2011)； E.Poreba et al., " viral-induced tumour formed in epigenetic mechanism (Epigenetic mechanisms in Virus-induced tumorigenesis) ",《Clinical trial embryology (Clin Epigenetics)》2(2)：233- 47.2011.In another embodiment, BET inhibitor is because it infects in the infection of latency T cell and latency monocyte HIV-1 ability is re-activated in model, it is possible to combined with antiretroviral therapy for treating HIV.J.Zhu et al., 《Cell is reported》(2012)；C.Banerjee et al.,《Leukocyte-biological magazine》(2012)；K.Bartholomeeusen etc. People,《Journal of biological chemistry》(2012)；Z.Li et al.,《Nucleic acids research》(2012).

In one embodiment, because work of the protein of epigenetic process and brominated domain in nervous disorders With, thus BET inhibitor Formulas I or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or Hydrate or composition comprising one or more of those compounds can be used for treating disease, including but not limited to Alzheimer disease, Parkinson's, Huntington disease (Huntington disease), anxiety disorder, schizophrenia, Rubens Smooth-taybi's syndrome (Rubinstein-Taybi syndrome) and epilepsy.R.Prinjha et al.,《Pharmaceutical science becomes Gesture》33(3)：146-53(2012)；S.Muller et al., " bromine domain is as therapy target (Bromodomains as Therapeutic targets) ",《Molecular medicine expert opinion (Expert Rev Mol Med)》13：e29(2011).

In one embodiment, because BRDT exhausts or suppressed the influence to spermatid development, BET inhibitor Formulas I Or Formula II compound or its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or hydrate or include those changes The composition of one or more of compound may be used as reversible male contraceptive pill.M.Matzuk et al., " little molecules in inhibiting BRDT is so as to male contraception ",《Cell》150(4)：The 673-684 pages (2012)；B.Berkovits et al., " containing double bromine structures The testis specific protein matter BRDT in domain forms compound with multiple spliceosome component and cut for the mRNA in circular spermatid Connect with 3 '-UTR truncate needed for ",《Nucleic acids research》40(15)：7162-75(2012).

Pharmaceutical composition

The pharmaceutical composition of the present invention includes at least one and prepared together with one or more pharmaceutically acceptable supporting agents Formulas I or Formula II compound as described herein or its dynamic isomer, stereoisomer, pharmaceutically acceptable salt or water Compound.These preparations include being suitable for oral, per rectum, are local, buccal and not enteral (for example, subcutaneous, intramuscular, skin It is interior or intravenous) dispensing preparation.Most suitable types of administration is by the journey depending on symptom to be treated under any particular cases The property of degree and seriousness and specific compound used.

The preparation for being suitable for being administered orally can be rendered as discrete unit, such as capsule, flat jelly, buccal tablet or tablet, Each the compounds of this invention containing scheduled volume, it is in powder or particle form；In the solution in water-based or non-aqueous liquid or Form of suspension；Or in oil-in-water or water-in-oil emulsion form.As noted, this kind of preparation can pass through any suitable medicine Prepared by method, the described method comprises the following steps：Using at least one the compounds of this invention and supporting agent as reactive compound Or excipient (it may be constructed one or more accessory ingredients) is joined together.Supporting agent compatible with other compositions of preparation and Must be acceptable in the sense that harmless to recipient.Supporting agent can be solid or liquid or all right, or can use herein Described at least one compound is formulated as the reactive compound in unit dose preparation, such as tablet, and it can contain about At least one reactive compounds of the 0.05 weight % to about 95 weight %.There can also be other pharmacologically active materials, wrap Include other compounds.The preparation of the present invention can be prepared by any of well-known pharmaceutical technology, the pharmacy Technology is substantially made up of mixing each component.

Relevant solid composite, Conventional nontoxic solid supporting agent include such as pharmaceutical grade mannitol, lactose, starch, tristearin Sour magnesium, saccharin sodium, talcum, cellulose, glucose, sucrose, magnesium carbonate etc..Pharmacologically can administration fluid composition citing For can for example, by by least one reactive compound as of the invention described herein and optional pharmaceutical adjuvants dissolving Or be dispersed in such as water, physiological saline, aqueous dextrose, glycerine, ethanol excipient, so as to form solution or suspension to make It is standby.In general, suitable preparation can be by mixing uniformly and nearly at least one reactive compound of the invention With liquid or Fine-powdered solids supporting agent or both, and then it is molded product if necessary.For example, can by compression or Powder or the particle of at least one the compounds of this invention are moulded to prepare tablet, the compounds of this invention can optionally with it is a kind of or A variety of accessory ingredient combinations.Compressed tablets can be at least one free in such as powder or particle by being compressed in suitable machine It is prepared by the compounds of this invention of liquid form, the compounds of this invention can optionally with adhesive, lubricant, inert diluent And/or surface-active/dispersant.Molded tablet can be by moulding to be made, in the machine in suitable machine In, with least one the compounds of this invention of inert liquid diluent moistening powdery form.

Being suitable for the preparation of buccal (sublingual) administration includes buccal tablet and lozenge, and buccal tablet includes at least one present invention Compound is in flavoured base, and typically sucrose and Arabic gum or the Radix Astragali, lozenge include at least one compound in inertia base In matter, such as gelatin and glycerine or sucrose and Arabic gum.

The preparation of the present invention for being suitable for not enteral administration includes at least one Formulas I or Formula II compound or its mutually variation Structure body, stereoisomer, the sterile aqueous formulation of pharmaceutically acceptable salt and hydrate, its blood with intended recipient It is substantially isotonic.The intravenous administration of these preparations, but dispensing can also be realized by means of subcutaneous, intramuscular or intracutaneous injection.This Class preparation can conveniently by least one compound as described herein is mixed with water and cause resulting solution it is sterile simultaneously And with blood is isotonic prepares.About 0.1 active ingredient for arriving about 5%w/w can be contained according to the Injectable composition of the present invention Thing.

The preparation for being suitable for per rectum administration is rendered as unit dose suppositories.These suppositorys can be by will be such as this paper institutes At least one compound stated mixes with one or more Conventional solid supporting agents (such as cocoa butter), and then mixes gained Thing is molded to prepare.

The preparation for being suitable for locally applying to skin can be in ointment, emulsifiable paste, lotion, paste, gel, spraying, aerosol Agent or oil form.The supporting agent and excipient that can be used are including vaseline, lanolin, polyethylene glycol, alcohol and both or more The combination of more persons.Reactive compound (that is, at least one Formulas I or Formula II compound or its dynamic isomer, stereoisomer, medicine Acceptable salt and hydrate on) typically arrive about 15%w/w with about the 0.1% of composition, e.g., from about 0.5 to about 2% Concentration is present.

The administration amount of reactive compound can depend on subject to be treated, the body weight of subject, administration mode and The judgement of prescriber.For example, dosage regimen can be related to daily or per half a day with about 1 μ g to about 1000mg perception agents Measure administration potting compound.In another embodiment, can use such as the intermittent administration doses such as monthly or every year Potting compound.Encapsulation is conveniently accessible to action site and allows administration active component simultaneously, produces cooperative effect in theory.Root According to standard administration regimens, doctor is by easy judgement optimal dose and can easily change dispensing to realize this kind of dosage.

Compound described herein or the therapeutically effective amount of composition can be by the treatment validity of compound come degree Amount.However, dosage can depend on the demand of patient, the severity for the symptom treated and compound used therefor and change. In one embodiment, the disclosed compound of therapeutically effective amount is enough to establish maximal plasma concentration.Preliminary doses such as such as basis Animal testing determines, and is carried out for the adjustment of the dosage of mankind's administration according to the acceptable specification in this area.

Toxicity and therapeutic efficiency can be determined by the standard pharmaceutical procedures in cell culture or experimental animal, such as be determined LD₅₀(the lethal dosage of colony for making 50%) and ED₅₀(the 50% effective dosage of mass treatment).Toxicity and therapeutic action it Between dose ratio for therapeutic index and it can be expressed as ratio LD₅₀/ED₅₀.The composition for showing big therapeutic index is preferred 's.

The data obtained from cell culture assays or zooscopy can be used for preparing multiple dosage suitable for the mankind. The treatment effective dose realized in one animal model can use conversion factor as known in the art by conversion for In another animal, including the mankind (on equivalency tables area dose factor, see, for example, Freireich et al.,《Cancer chemotherapy report Accuse (Cancer Chemother.Reports)》50(4)：219-244 (1966) and table 1).

The equivalency tables area dose factor of table 1.：

The dosage of this kind of compound is preferably including ED₅₀In the range of circulation composition inside, and with extremely low toxicity or It is non-toxic.Dosage can depend on formulation used and dosing way used and change in the range of this.In general, treatment has Effect amount can change with the severity of the age of subject, the patient's condition and sex and the medical condition of subject.Dosage can To be determined by doctor and be adjusted as needed the therapeutic action to be adapted to observed.

In one embodiment, Formulas I or Formula II compound or its dynamic isomer, stereoisomer, pharmaceutically acceptable Salt or hydrate or the composition comprising one or more of those compounds combine administration with another therapeutic agent.Phase For the compound or composition of the independent administration present invention, other therapeutic agents can provide cumulative or Synergistic gains.Therapeutic agent can To be such as Statins (statin)；PPAR activators, such as thiazolidinedione or fibrates (fibrate)；Nicotinic acid, RVX, FXR or lxr agonist；Bile acid reuptaking inhibitor；Cholesterol absorption inhibitor；Inhibitors of cholesterol synthesis；Cholesteryl ester Transport protein (CETP), ion exchange resin；Antioxidant；(ACAT suppresses the inhibitor of acetyl-CoA cholesterol acyltransferase Agent)；Tyrphostin (tyrophostine), the medicine based on sulfonylureas；Biguanides；Alpha-glucosidase inhibitor； Apo E regulatory factor；HMG-CoA reductase inhibitor, microsomal triglyceride transfer protein；LDL medicines drop；Rise HDL medicines；HDL reinforcing agents；The regulatory factor of Apolipoprotein A-IV and/or Apolipoprotein genes；Or any cardiovascular drugs.

In another embodiment, Formulas I or Formula II compound or its dynamic isomer, stereoisomer, can pharmaceutically connect The salt or hydrate received or the composition comprising one or more of those compounds combine throwing with one or more antiphlogistics With.Antiphlogistic can include immunodepressant, tnf inhibitor, corticosteroid, non-steroidal anti-inflammatory drug (NSAID), improvement disease Feelings antirheumatic drug (DMARD) etc..Exemplary antiphlogistic includes such as metacortandracin；Methylprednisolone (methylprenisolone)Fluoxyprednisolone (triamcinolone), methotrexate (MTX) (methotrexate)HCQSalicylazosulfapyridine (sulfasalzine)Leflunomide (leflunomide)Etanercept (etanercept)Ying Li Former times monoclonal antibody (infliximab)Adalimumab (adalimumab)RituximabOrencia (abatacept)Il-1, anakinra (anakinra) (Kineret^TM), brufen (ibuprofen), Ketoprofen (ketoprofen), fenoprofen (fenoprofen), Nabumetone Raw (naproxen), Aspirin (aspirin), acetaminophen (acetominophen), Indomethacin (indomethacin), Sulindac (sulindac), Meloxicam (meloxicam), piroxicam (piroxicam), tenoxicam (tenoxicam), Lornoxicam (lornoxicam), ketorolac (ketorolac), Etodolac (etodolac), mefenamic acid (mefenamic Acid), Meclofenamic Acid (meclofenamic acid), Flufenamic acid (flufenamic acid), Tolfenamic Acid (tolfenamic acid), Diclofenac (diclofenac), Oxaprozins (oxaprozin), apazone (apazone), Buddhist nun Mei Shuli (nimesulide), Nabumetone (nabumetone), Tenidap (tenidap), Etanercept (etanercept), tolmetin (tolmetin), bute (phenylbutazone), Oxyphenbutazone (oxyphenbutazone), Diflunisal (diflunisal), salsalate (salsalate), Olsalazine Or salicylazosulfapyridine (olsalazine).

The inventory of exemplary embodiments

1. a kind of compound of formula I,

Wherein：

R₄Selected from hydrogen, optionally by 1 to 5 independently selected from R₅Group substitution alkyl (C₁-C1₀), carbocyclic ring (C₃-C₁₀) with And heterocycle (C₂-C1₀)；

Each R₅Independently selected from deuterium, epoxides, alkyl (C₁-C₆), alkoxy (C₁-C₆), amino ,-NHC (O) NH- alkyl (C₁-C₆), halogen, acid amides ,-CF₃、-CN、-N₃, ketone (C₁-C₆) ,-S (O)-alkyl (C₁-C₄)、-SO₂- alkyl (C₁-C₆), sulfane Base (C₁-C₆) ,-COOH and ester, it each can be optionally by oxirane, hydrogen, F, Cl, Br ,-OH ,-NH₂、-NHMe、- OMe ,-SMe, oxo and/or thioxo-oxo substitution；

Y is selected from-N- ,-CH- and-CNH₂-。

2. a kind of Formula II compound,

Wherein：

Z is selected from hydrogen and amino.

3. according to embodiment 1 or the compound of embodiment 2, wherein R₁Selected from optionally by 1 to 5 independently selected from R₅Group Substituted carbocyclic ring (C₅-C₁₀)。

4. the compound of any one in embodiment 1 to 3, wherein R₁Selected from optionally by 1 to 5 independently selected from R₅'s The phenyl of group substitution.

5. the compound of any one in embodiment 1 to 4, wherein R₁Selected from by 1 to 5 independently selected from R₅Group take The phenyl in generation.

6. the compound of any one in embodiment 1 to 5, wherein R₁Selected from by 1 to 5 independently selected from epoxides, Alkyl (C₁-C₆), halogen and ketone (C₁-C₆) group substitution phenyl, these groups each can optionally by oxirane, Hydrogen, F, Br and/or Cl substitution.

7. the compound of any one in embodiment 1 to 6, wherein R₁Selected from by 1 to 5 independently selected from oxirane, Methyl, ethyl, F and acetyl group group substitution phenyl, these groups optionally can each substitute by oxirane and Cl.

8. the compound of any one in embodiment 1 to 7, wherein R₁Selected from by oxirane, methyl oxirane, halogen Ketone (C₁-C₆) and/or alkylhalide group (C₁-C₆) substitution phenyl.

9. the compound of any one in embodiment 1 to 8, wherein R₁It is selected from：

Wherein benzyl ring is optionally further by 1 to 4 independently selected from R₅Group substitution.

10. the compound of any one in embodiment 1 to 9, wherein R₁It is selected from：

Wherein benzyl ring is optionally further optionally substituted by halogen.

11. the compound of any one in embodiment 1 to 10, wherein R₁It isWherein benzyl ring is appointed Selection of land is further by 1 to 4 independently selected from R₅Group substitution.

12. the compound of any one in embodiment 1 to 11, wherein R₁It isWherein benzyl ring is appointed Selection of land is further optionally substituted by halogen.

13. the compound of any one in embodiment 1 to 12, wherein R₁It is

14. the compound of any one in embodiment 1 to 13, wherein R₁It is selected from：

It is optionally by 1 to 4 independently selected from R₅Group substitution.

15. the compound of any one in embodiment 1 to 14, wherein R₁It is selected from：

16. the compound of any one in embodiment 1 to 15, wherein R₁It is selected from：

17. according to embodiment 1 or the compound of embodiment 2, wherein R₁Selected from optionally by 1 to 5 independently selected from R₅Base Heterocycle (the C of group's substitution₂-C₁₀)。

18. according to the compound of any one in embodiment 1,2 and 17, wherein R₁Selected from by oxirane, methyl oxirane, Halogen ketone (C₁-C₆) and/or alkylhalide group (C₁-C₆) substitution 5-6 circle heterocycles.

19. the compound of any one in embodiment 1 to 18, wherein R₂It is methyl and R₃Selected from optionally by halogen and Alkyl (the C of hydroxyl substitution₁-C₆)。

20. the compound of any one in embodiment 1 to 19, wherein R₂And R₃It is methyl.

21. the compound of any one in embodiment 1 to 20, wherein R₄Selected from hydrogen and optionally independently selected by 1 to 5 From R₅Group substitution alkyl (C₁-C₆)。

22. the compound of any one in embodiment 1 to 21, wherein R₄It is hydrogen.

23. the compound of any one in embodiment 1 to 21, wherein R₄Selected from optionally by 1 to 5 independently selected from R₅ Group substitution alkyl (C₁-C₆)。

24. the compound of any one in embodiment 1 to 21 and 23, wherein R₄It is methyl.

25. the compound of any one in embodiment 1 to 19, wherein R₄Selected from optionally by 1 to 5 independently selected from R₅ Group substitution heterocycle (C₂-C₆)。

26. the compound of any one in embodiment 1 to 19, wherein R₄Selected from optionally by 1 to 5 independently selected from R₅ Group substitution carbocyclic ring (C₃-C₁₀)。

27. the compound of any one in embodiment 1 to 26, wherein each R₅Independently selected from deuterium, epoxides, alkyl (C₁-C₆), amino ,-NHC (O) NH- alkyl (C₁-C₆), halogen, acid amides ,-CF₃、-CN、-N₃, ketone (C₁-C₆) ,-S (O)-alkyl (C₁-C₄)、-SO₂Alkyl (C₁-C₆) and sulfanyl (C₁-C₆)。

28. the compound of any one in embodiment 1 to 27, wherein Y are-CH-.

29. the compound of any one in embodiment 1 to 27, wherein Y are-N-.

30. the compound of any one in embodiment 1 to 27, wherein Y are-C (NH₂)-。

31. according to the compound of embodiment 1, wherein X is-CH₂-。

32. according to the compound of embodiment 1, wherein Z is hydrogen.

33. according to the compound of embodiment 1, wherein Z is-NH₂。

34. according to embodiment 1 or the compound of embodiment 2, wherein the Formulas I or Formula II compound are selected from：

5- (dimethyl -1,2- oxazole -4- bases) -1- (the fluoro- 4- of 3- (oxirane -2- bases) benzyl) pyridine -2 (1H) -one；

5- (dimethyl -1,2- oxazole -4- bases) -1- { [4- (oxirane -2- bases) phenyl] methyl } -1,2- dihydropyridines -2- Ketone；

3- amino -5- (the different diazole -4- bases of 3,5- dimethyl) -1- (4- (oxirane -2- bases) benzyl) pyridine -2 (1H) - Ketone；

6- (dimethyl -1,2- oxazole -4- bases) -1- { [4- (oxirane -2- bases) phenyl] methyl } -1H-1,3- benzodiazoles - 4- amine；

4- (1- { [4- (2- chloroethyls) phenyl] methyl } -2- methyl isophthalic acid H- imidazos [4,5-b] pyridine -6- bases) -3,5- diformazans Base -1,2- oxazole；

The chloro- 1- of 2- (4- { [6- (dimethyl -1,2- oxazole -4- bases) -2- methyl isophthalic acid H- imidazos [4, the 5-b] base of pyridine -1] first Base } phenyl) second -1- ketone；

3,5- dimethyl -4- (2- methyl isophthalic acids-{ [4- (oxirane -2- ylmethyls) phenyl] methyl } -1H- imidazos [4,5-b] Pyridine -6- bases) -1,2- oxazoles；And

Its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or hydrate.

35. a kind of pharmaceutical composition, the compound comprising any one in embodiment 1 to 34 and pharmaceutically acceptable load Agent.

A kind of 36. method for being used to suppress BET protein functions, comprising administration therapeutically effective amount according in embodiment 1 to 34 The compound of any one or the pharmaceutical composition according to embodiment 35.

37. a kind of method for treating the LADA relevant with BET protein or inflammatory conditions, effective comprising administration treatment The compound or the pharmaceutical composition according to embodiment 35 of any one in embodiment 1 to 34 of amount.

38. according to the method for embodiment 37, wherein the LADA or inflammatory conditions are selected from acute disseminated myelencephalon Inflammation, agammaglobulinemia, anaphylactia, stiff property spondylitis, the anti-TBM ephritis of anti-GBM/, antiphospholipid syndrome, itself Immunologic aplastic anemia, oneself immunity hepatitis, Autoimmune Inner Ear Disease, autoimmune myocarditis, itself exempt from Epidemic disease pancreatitis, autoimmune retinopathy, autoimmune thrombocytopenic purpura, Behcet's disease, epidermolysis class day blister Sore, castleman's disease, chylous diarrhea, churg-Strauss syndrome, Crohn's disease, Ke's radicular syndrome, dry eye syndrome, primary Mixed type cryoglobulinemia, dermatomyositis, devic's disease, encephalitis, eosinophilic esophagitis, eosinophilic fasciitis, erythema nodosum, Giant cell arteritis, glomerulonephritis, goodpasture's syndrome, granulomatous Polyangiitis (Wegener), Robert Graves Disease, Guillain-Barre＆1＆ syndrome, Hashimoto's thyroiditis, hemolytic anemia, purpura,Henoch-Schonlein, idiopathic pulmonary fibrosis, IgA Nephrosis, inclusion body myositis, type i diabetes, interstitial cystitis, Kawasaki disease, leukocytoclastic angiitis, lichen planus, wolf Sore (SLE), microscopic polyangitis, multiple sclerosis, myasthenia gravis, myositis, optic neuritis, pemphigus, POEMS are comprehensive It is simulator sickness, PAN, PBC, psoriasis, arthritic psoriasis, pyoderma gangraenosum, multiple Hair property polychondritis, rheumatoid arthritis, sarcoidosis, chorionitis, Sjogren syndrome, takayasu's arteritis, transverse ridge Marrow inflammation, ulcerative colitis, uveitis and leucoderma.

A kind of 39. acute or chronic non-self immune inflammatory illness treated characterized by IL-6 and/or IL-17 imbalance Method, the compound of any one in embodiment 1 to 34 comprising administration therapeutically effective amount or according to embodiment 35 Pharmaceutical composition.

40. according to the method for embodiment 39, wherein the acute or chronic non-self immune inflammatory illness be selected from nasosinusitis, Pneumonia, osteomyelitis, gastritis, enteritis, gingivitis, appendicitis, irritable colon syndrome, tissue transplantation rejection reaction, COPD Property tuberculosis (COPD), septic shock, osteoarthritis, acute gout, ALI, acute renal failure, burn, herxheimer reaction And the SIRS relevant with viral infection.

41. according to the method for embodiment 39, wherein the acute or chronic non-self immune inflammatory illness is selected from rheumatoid Property arthritis (RA) and multiple sclerosis (MS).

42. a kind of treat the cancer relevant with overexpression, transposition, amplification or the restructuring for suppressing sensitive myc families cancer protein to BET The method of disease, the compound of any one in embodiment 1 to 34 comprising administration therapeutically effective amount or according to embodiment 35 Pharmaceutical composition.

43. a kind of method for treating the cancer relevant with the overexpression of BET protein, transposition, amplification or restructuring, is controlled comprising administration Treat the compound of any one in embodiment 1 to 34 of effective dose or the pharmaceutical composition according to embodiment 35.

44. one kind treatment adjusts the cancer of oncogene dependent on pTEFb (Cdk9/ cyclin T) and BET protein Method, the compound of any one in embodiment 1 to 34 comprising administration therapeutically effective amount or according to embodiment 35 Pharmaceutical composition.

45. a kind of method for treating the cancer relevant with BET response genes CDK6, Bc12, TYRO3, MYB and hTERT up-regulation, The compound of any one in embodiment 1 to 34 comprising administration therapeutically effective amount or the drug regimen according to embodiment 35 Thing.

46. a kind of method for treating the cancer relevant with the gene adjusted by super enhancer, includes administration therapeutically effective amount The compound of any one in embodiment 1 to 34 or the pharmaceutical composition according to embodiment 35.

A kind of 47. method for treating the cancer sensitive to BET inhibitory action, comprising administration therapeutically effective amount according to embodiment 1 The compound of any one in 34 or the pharmaceutical composition according to embodiment 35.

48. a kind of treat to the side with immunotherapy, hormonal deprivation and/or the resistant cancer of regimen chemotherapy Method, the compound of any one in embodiment 1 to 34 comprising administration therapeutically effective amount or the medicine according to embodiment 35 Composition.

49. the method for any one in embodiment 36 to 48, wherein the compound of any one in embodiment 1 to 34 Or combined according to the pharmaceutical composition of embodiment 35 with other therapies, chemotherapeutant or antiproliferative.

50. according to the method for embodiment 49, wherein the therapeutic agent is selected from ABT-737, azacitidine (Victor bundle), AZD1152 (Barasertib), AZD2281 (olaparib), AZD6244 (U.S. of department replaces Buddhist nun), BEZ235, bleomycin sulfate, bortezomib (Bortezomib), busulfan (bridle blue), camptothecine, cis-platinum, endoxan (carat is fragrant), CYT387, cytarabine (Ara-C), reach Carbazine, DAPT (GSI-IX), Decitabine, dexamethasone, adriamycin (A Deli mycins), Etoposide, everolimus (RAD001), Flavopiridol (Avobenzene west ground), Jia Litepi (STA-9090), Gefitinib (Iressa), idarubicin, different ring Phosphamide (rice support is celestial), IFNa2a (Recomvinated Interferon α-2a A), melphalan (L-Sarcolysinum), plum plug azoles Lars lead to (Temozolomide), diformazan pair Guanidine, mitoxantrone (Novantrone), taxol, insoral, PKC412 (midostaurin), PLX4032 (Wei Luofeini), pool Ma Du Amine (CC-4047), metacortandracin (delta pine), rapamycin, Revlimid (lenalidomide), Luso profit replace Buddhist nun (INCB018424), (peace can for Sorafenib (Nexavar), SU11248 (Sutent), SU11274, vincaleukoblastinum, vincristine It is flat), vinorelbine (NVB), Vorinostat (SAHA) and WP1130 (wearing lattice Racine).

51. a kind of method for treating benign proliferative or fibrotic conditions, the benign proliferative or fibrotic conditions be selected from by The group of consisting of：Benign soft tissue neoplasm, bone tumour, brain and tumor of spinal cord, eyelid and orbital tumor, granuloma, fat Knurl, meningioma, Multiple Endocrine neoplasia, nasal polyp, pituitary tumor, prolactinoma, pseudotumor cerebri, seborrheic keratosis, Polyp of stomach, thyroid nodule, pancreas capsule anything superfluous or useless, hemangioma, vocal nodule, polyp and tumour, castleman's disease, chronic Tibetan hair Disease, histiocytoma, pilar cyst, pyogenic granuloma, juvenile polyposis syndrome, idiopathic pulmonary fibrosis, kidney fiber Change, postoperative stenosis, keloid is formed, chorionitis and cardiac fibrosis, methods described include the root of administration therapeutically effective amount Compound according to any one in embodiment 1 to 34 or the pharmaceutical composition according to embodiment 35.

52. a kind of treat the method for benefiting from up-regulation or the disease or illness of ApoA-I transcriptions and protein expression, administration is included The compound of any one in embodiment 1 to 34 of therapeutically effective amount or the pharmaceutical composition according to embodiment 35.

53. according to the method for embodiment 52, wherein the disease is angiocardiopathy, dyslipidemia, atherosclerosis, high courage Sterol mass formed by blood stasis, metabolic syndrome and Alzheimer disease.

A kind of 54. method for treating the cancer relevant with virus, comprising administration therapeutically effective amount according in embodiment 1 to 34 The compound of any one or the pharmaceutical composition according to embodiment 35.

55. a kind of method for treating HIV, individually or with what ART agent was combined controlled comprising administration Treat the compound of any one in embodiment 1 to 34 of effective dose or the pharmaceutical composition according to embodiment 35.

56. one kind is used to treat selected from Alzheimer disease, Parkinson's, Heng Yandun diseases, anxiety disorder, schizophrenia, Lu Bin The method of the disease or illness of Si Tan-taybi's syndrome and epilepsy, arrived comprising administration therapeutically effective amount according to embodiment 1 The compound of any one in 34 or the pharmaceutical composition according to embodiment 35.

57. a kind of male contraception method, the compound of any one in embodiment 1 to 34 comprising administration therapeutically effective amount Or the pharmaceutical composition according to embodiment 35.

Example

Unless otherwise noted, otherwise reagent and solvent are used universal method as former state as what is obtained from commercial supplier.In cloth Proton NMR spectral is obtained on Luke (Bruker) ADVANCE 300,400 or 500 spectrometers.Spectrum is represented with ppm (δ) And coupling constant J values are reported with hertz (Hz) for unit.Where appropriate, in water this (Waters) Aguity UPLC, Agilent (Agilent) 6130A, Applied Biosystems, Inc. (Applied Biosystems) API-150EX or Shimadzu (Shimadzu) Mass spectral analysis is carried out with ESI or APCI patterns on 2020 instruments.

Abridge .DBU：- 7- the alkene of 1,8- diazabicyclo [5.4.0] 11；DCM：Dichloromethane；DMF：Dimethyl formyl Amine；DMSO：Dimethyl sulfoxide；EtOAc：Ethyl acetate；NBS：N- bromo-succinimides；NCS：N- chlorosuccinimides； MeOH：Methanol；PE：Petroleum ether；THF：Tetrahydrofuran；TLC：Thin-layer chromatography.

Example 1：Prepare 5- (dimethyl -1,2- oxazole -4- bases) -1- (the fluoro- 4- of 3- (oxirane -2- bases) benzyl) pyridine -2 (1H) -one

By 4 (500mg, 2.44mmol), pyridine (578mg, 7.32mmol) and MsCl (559mg, 4.88mmol) in CH₂Cl₂ 16h is stirred at room temperature in reactant mixture in (10mL).Use CH₂Cl₂Diluted reaction mixture, and pass through one layer of diatomite Filter reactant mixture.Filtrate is concentrated, obtains the compound 5 (4.2g, 95%) in pale solid shape：¹H NMR (500MHz, CDCl₃) δ 7.63-7.43 (m, 3H), 6.31 (s, 2H).

According to literature procedure (WO 2014096965, compound 14) prepare compound 3.

By 5- (the different diazole -4- bases of 3,5- dimethyl) pyridine -2 (1H) -one 3 (285mg, 1.5mmol), the bromo- 4- (chloromethanes of 1- Base) -2- fluorobenzene 5 (368mg, 1.65mmol) and K₂CO₃(414mg, 3.0mmol) is in CH₃Mixture in CN (10mL) is at 70 DEG C Lower stirring 16h.Reactant mixture is cooled to room temperature and filtered by one layer of diatomite.Filtrate is concentrated and on silica gel Purifying, obtain the desired product 6 (180mg, 32%) in pale solid shape.¹H NMR (300MHz, CDCl₃)δ7.59-7.54 (m, 1H), 7.30-7.26 (m, 2H), 7.17-7.12 (m, 2H), 7.03 (d, J=8.1Hz, 1H), 5.14 (s, 2H), 2.36 (s, 3H), 2.22 (s, 3H)；ESI MS m/z378[M+H]⁺。

Into solution of 6 (180mg, the 0.48mmol) in DMF (5mL) add tributyl (vinyl) stannane (197mg, 0.62mmol) and Pd (PPh₃)₂Cl₂(34mg, 0.048mmol).Reactant mixture is purified with nitrogen and is heated at 85 DEG C 16h.Mixture is filtered by one layer of diatomite.Concentrate filtrate.Pass through chromatogram (silica gel, 0-40% ethyl acetate/dichloromethanes) Purifying, obtain 7 (83mg, 53%) in orange oily：¹H NMR (300MHz, CDCl₃) δ 7.51-7.46 (m, 1H), 7.26- 7.25 (m, 1H), 7.14 (d, J=1.8Hz, 1H), 7.09-7.00 (m, 2H), 6.91-6.74 (m, 2H), 5.82 (d, J= 17.7Hz, 1H), 5.40 (d, J=11.1Hz, 1H), 5.15 (s, 2H), 2.32 (s, 3H), 2.18 (s, 3H)；ESI MS m/ z325[M+H]⁺。

At 0 DEG C, into solution of 7 (83mg, the 0.26mmol) in acetone (3mL) and water (1mL) add NBS (50mg, 0.29mmol).Reactant mixture 6h is stirred at room temperature.At 0 DEG C, into thing mixed above add NaOH (21mg, 0.52mmol), and it is stirred at room temperature 16h.Reactant mixture is filtered by one layer of diatomite.Concentrate filtrate.Pass through color (silica gel, 0-40% ethyl acetate/dichloromethanes) purifying is composed, obtains the example 1 (53mg, 60%) in pale solid shape.¹H NMR (500MHz, DMSO-d₆) δ 7.94 (d, J=2.5Hz, 1H), 7.50 (dd, J=9.0,2.5Hz, 1H), 7.24 (d, J= 11.5Hz, 1H), 7.19-7.17 (m, 2H), 6.51 (d, J=9.0Hz, 1H), 5.12 (s, 2H), 4.08 (dd, J=4.0, 2.5Hz, 1H), 3.14 (dd, J=5.5,4.0Hz, 1H), 2.87 (dd, J=5.5,2.5Hz, 1H), 2.36 (s, 3H), 2.19 (s, 3H)；ESI m/z341[M+H]⁺；HPLC98.1%.

Example 2：Prepare 5- (dimethyl -1,2- oxazole -4- bases) -1- { [4- (oxirane -2- bases) phenyl] methyl } -1,2- bis- Pyridinium hydroxide -2- ketone

Example 2 is prepared according to the program similar with example 3.The analyze data of example 2：¹H NMR (300MHz, CDCl₃)δ 7.40-7.12 (m, 6H), 6.64 (d, J=9.3Hz, 1H), 5.17 (s, 2H), 3.85-3.84 (m, 1H), 3.16-3.13 (m, 1H), 2.78-2.74 (m, 1H), 2.30 (s, 3H), 2.15 (s, 3H)；ESI MSm/z323[M+H]⁺

Example 3：Prepare 3- amino -5- (the different diazole -4- bases of 3,5- dimethyl) -1- (4- (oxirane -2- bases) benzyl) pyrrole Pyridine -2 (1H) -one

According to literature procedure (WO 2014096965, p82, chapters and sections 000205, compound 30) prepare compound 1.

By compound 1 (100mg, 0.49mmol), 2- (4- (chloromethyl) phenyl) oxirane 2 (90mg, 0.54mmol) And K₂CO₃(135mg, 0.98mmol) is in CH₃Mixture in CN (6mL) stirs 16h at 70 DEG C.Reactant mixture is cooled down Filtered to room temperature and by one layer of diatomite.Filtrate is concentrated and purified on silica gel, is obtained in pale solid shape Desired product example 3 (94mg, 57%).¹H NMR (300MHz, DMSO-d₆) δ 7.30 (dd, J=25.5,8.4Hz, 4H), 7.11 (d, J=2.1Hz, 1H), 6.44 (d, J=2.4Hz, 1H), 5.28 (s, 2H), 5.12 (s, 2H), 3.90 (dd, J=4.2, 2.7Hz, 1H), 3.09 (dd, J=5.4,4.2Hz, 1H), 2.81 (dd, J=5.4,2.7Hz, 1H), 2.34 (s, 3H), 2.17 (s, 3H)；ESI MS m/z 338[M+H]⁺；HPLC purity ＞ 99%.

Example 4：6- (dimethyl -1,2- oxazole -4- bases) -1- { [4- (oxirane -2- bases) phenyl] methyl } -1H-1,3- benzene And diazole -4- amine

By 16 (1.0g, 4.7mmol), 3 (4.5g, 6.6mmol), K₂CO₃(1.3g, 9.4mmol), the dioxane of Isosorbide-5-Nitrae- The mixture of (48mL) and water (3.5mL) with nitrogen deaerate 20 minutes, then add tetrakis triphenylphosphine palladium (0) (550mg, 0.94mmol).Mixture is heated 18 hours at 90 DEG C, is then cooled to room temperature.By chromatogram (silica gel, 0-10% methanol/ Dichloromethane) purifying crude product mixture, obtain 17 (760mg, 68%) in pale solid shape：¹H NMR (500MHz, CDCl₃) δ 7.98 (s, 1H), 6.74 (s, 1H), 6.40 (s, 1H), 4.45 (s, 2H), 2.38 (s, 3H), 2.25 (s, 3H)； ESIm/z229[M+H]+。

To 17 (100mg, 0.44mmol) in CH₃Potassium carbonate (121mg, 0.88mmol) is added in solution in CN (5mL) With 2- (4- (chloromethyl) phenyl) oxirane (81mg, 0.48mmol).The stirring reaction mixture 16h at 60 DEG C.Use dichloro Methane (20mL) diluted mixture and pass through one layer of diatomite and filter.Filtrate is concentrated and passes through chromatogram (silica gel, 0-10% CH₃OH/CH₂Cl₂) purifying, then purified by anti-phase comiflash, obtain in pale solid shape example 4 (70mg, 44%)：¹H NMR (300MHz, CD₃OD) δ 8.18 (s, 1H), 7.27 (s, 4H), 6.55 (d, J=1.2Hz, 1H), 6.45 (d, J =1.5Hz, 1H), 5.44 (s, 2H), 3.84 (dd, J=4.2,2.7Hz, 1H), 3.09 (dd, J=5.4,4.2Hz, 1H), 2.74 (dd, J=5.4,2.7Hz, 1H), 2.24 (s, 3H), 2.14 (s, 3H)；ESI MS m/z 361[M+H]⁺；HPLC purity 97.3%.

Example 5：4- (1- (4- (2- chloroethyls) benzyl) -2- methyl isophthalic acid H- imidazos [4,5-b] pyridine -6- bases) -3 is prepared, 5- dimethyl isoxazoles

Jiang the compound 5 (4.0g, 21.3mmol, 1.0 equivalent) in dioxane (60mL) and water (20mL), (3,5- diformazans Isoxazole -4- bases) boric acid (4.5g, 31.9mmol, 1.5 equivalent), K₂CO₃(5.9g, 42.6mmol, 2.0 equivalent) and Pd (PPh₃)₄(1.2g, 1.1mmol, 0.05 equivalent) is deaerated with nitrogen, and then heats 16h at 90 DEG C.By reactant mixture Distribution is between water (50mL) and EtOAc (50mL).Wash, organic phase separation through Na with water (50mL)₂SO₄Dry, filtering And concentrate under reduced pressure.Residue is purified by column chromatography (50-100%EtOAc/PE), obtains the change in yellow solid Compound 6 (3.2g, 15.7mmol, yield 74%)：¹H NMR (400MHz, CDCl₃) δ 2.26 (s, 3H), 2.40 (s, 3H), 3.42 (br.s., 2H), 4.34 (br.s., 2H), 6.80 (d, J=1.88Hz, 1H), 7.58 (d, J=1.88Hz, 1H).

To 6 (300mg, 1.5mmol, 1.0 equivalents) and 4- (2- ethoxys) benzaldehyde (221mg, 1.5mmol, 1.0 equivalent) Acetic acid (200 μ L) is added in solution in 1,2- dichloroethanes (15mL).Mixture 16h is stirred at 20 DEG C.Reaction is mixed Compound is distributed in DCM (15mL) and saturation NaHCO₃Between the aqueous solution (15mL).By organic phase separation, washed with water (15mL), Through [Na₂SO₄] dry, filter and concentrate under reduced pressure.Residue is purified by column chromatography (10-50%EtOAc/PE), obtained In the compound 7 (300mg, 892 μm of ol, yield 61%) of yellow solid.

At 20 DEG C, added portionwise into solution of 7 (300mg, 892 μm of ol, 1.0 equivalents) in MeOH (40mL) NaBH₄(101mg, 2.7mmol, 3.0 equivalent).Mixture 2h is stirred at 20 DEG C.It is quenched by adding water (15mL) at 0 DEG C Reactant mixture.Extracted again with water (20mL) diluted reaction mixture and with EtOAc (2 × 20mL).By organic portion of merging Divide and washed with water (20mL), through Na₂SO₄Dry, filter and concentrate under reduced pressure.Pass through column chromatography (50-100%EtOAc/ PE residue) is purified, obtains the compound 8 (300mg, 887 μm of ol, yield 99%) in yellow solid：¹H NMR (400MHz, CDCl₃) δ 2.08-2.15 (m, 3H), 2.26-2.31 (m, 3H), 2.90 (t, J=6.59Hz, 2H), 3.75 (br.s., 1H), 3.89 (t, J=6.59Hz, 2H, 4.33 (s, 4H), 6.62 (d, J=1.88Hz, 1H), 7.24-7.28 (m, 2H), 7.31-7.37 (m, 2H), 7.50 (d, J=1.88Hz, 1H).

Into solution of the compound 8 (300mg, 887 μm of ol, 1.0 equivalents) in 1,1,1- triethoxy ethane (10mL) Add sulfamic acid (861 μ g, 8.9 μm of ol, 0.01 equivalent).Mixture is stirred into 1h at 100 DEG C, and then under reduced pressure Concentration.Residue is distributed in EtOAc (20mL) and saturation NaHCO₃Between the aqueous solution (15mL).By organic phase separation, water is used (20mL) is washed, through Na₂SO₄Dry, filter and concentrate under reduced pressure.Purified by column chromatography (50-100%EtOAc/PE) Residue, obtain the compound 9 (100mg, 276 μm of ol, yield 31%) in yellow solid：¹H NMR (400MHz, CDCl₃)δ 2.19 (s, 3H), 2.36 (s, 3H), 2.72 (s, 3H), 2.88 (t, J=6.53Hz, 2H), 3.87 (t, J=6.59Hz, 2H), 5.35 (s, 2H), 7.05 (d, J=8.03Hz, 2H), 7.24 (d, J=8.03Hz, 2H), 7.32 (d, J=2.01Hz, 1H), 8.39 (d, J=1.88Hz, 1H).

Thionyl chloride is added into solution of the compound 9 (100mg, 276 μm of o1,1.0 equivalents) in DCM (10mL) (98mg, 828 μm of ol, 3.0 equivalents).Mixture is stirred into 1h at 20 DEG C, now LC/MS is shown, 9 are consumed completely.Subtracting Concentrated reaction mixture is depressed, and by residue distribution between water (15mL) and EtOAc (15mL).By organic phase separation, Washed with water (15mL), through Na₂SO₄Dry, filter and concentrate under reduced pressure.Pass through preparative TLC (10%MeOH/EtOAc) Purify residue, obtain in oily 4- (1- (4- (2- chloroethyls) benzyl) -2- methyl isophthalic acid H- imidazos [4,5-b] pyridine - 6- yls) -3,5- dimethyl isoxazoles (example 5) (46mg, 118 μm of ol, yield 43%, purity 98%)：¹H NMR (400MHz, CDCl₃) δ 2.20 (s, 3H), 2.37 (s, 3H), 2.73 (s, 3H), 3.07 (t, J=7.03Hz, 2H), 3.72 (t, J= 7.03Hz, 2H), 5.37 (s, 2H), 7.07 (d, J=8.16Hz, 2H), 7.24 (d, J=8.16Hz, 2H), 7.31 (d, J= 1.88Hz, 1H), 8.42 (d, J=2.01Hz, 1H)；ESI m/z 381.1[M+1]⁺。

Example 6：Prepare 2- chloro- 1- (4- ((6- (the different diazole -4- bases of 3,5- dimethyl) -2- methyl isophthalic acid H- imidazos [4,5-b] pyrroles Pyridine -1- bases) methyl) phenyl) ethyl ketone

To compound 6 (2.5g, 12.2mmol, 1.0 equivalent) and 4- bromobenzaldehydes (2.3g, 12.2mmol, 1.0 equivalent) in Acetic acid (200 μ L) is added in solution in 1,2- dichloroethanes (30mL).Mixture 16h is stirred at 20 DEG C.Reaction is mixed Thing is distributed in DCM (15mL) and saturation NaHCO₃Between the aqueous solution (15mL).By organic phase separation, washed, passed through with water (15mL) Na₂SO₄Dry, filter and concentrate under reduced pressure.Residue is purified by column chromatography (10-50%EtOAc/PE), obtained in Huang The compound 7 (2.2g, 5.9mmol, yield 48%) of color solid-like：

At 20 DEG C, boron hydrogen is added portionwise into solution of 7 (2.2g, 5.9mmol, 1.0 equivalents) in MeOH (20mL) Change sodium (672mg, 17.8mmol, 3.0 equivalent).Mixture is stirred at 20 DEG C to 2h and by adding water at 0 DEG C (15mL) is quenched.Extracted again with water (50mL) diluted mixture and with EtOAc (2 × 40mL).The organic moiety of merging is used Water (40mL) washs, through Na₂SO₄Dry, filter and concentrate under reduced pressure.It is pure by column chromatography (50-100%EtOAc/PE) Change residue, obtain the compound 8 (1.8g, 4.8mmol, yield 81%) in yellow solid：¹H NMR (400MHz, CDCl₃) δ 2.12 (s, 3H), 2.28 (s, 3H), 3.79 (br.s., 1H), 4.33 (d, J=4.89Hz, 4H), 6.55 (d, J=1.63Hz, 1H), 7.26-7.31 (m, 2H), 7.46-7.56 (m, 3H).

1,1,1- tri- ethoxy is added into solution of the compound 8 (1.7g, 4.6mmol, 1.0 equivalent) in acetic acid (20mL) Base ethane (3.7g, 22.8mmol, 5.0 equivalent).Mixture is stirred into 1h at 100 DEG C, and then concentrated under reduced pressure.Will Residue is distributed in EtOAc (50mL) and saturation NaHCO₃Between the aqueous solution (50mL).By organic phase separation, washed with water (20mL) Wash, through Na₂SO₄Dry, filter and concentrate under reduced pressure.Residue is purified by column chromatography (50-100%EtOAc/PE), obtained To the compound 9 (1.6g, 4.0mmol, yield 88%) in yellow solid：¹H NMR (400MHz, CDCl₃)δ2.18-2.24 (m, 3H), 2.33-2.39 (m, 3H), 2.67-2.74 (m, 3H), 5.34 (s, 2H), 6.97 (d, J=8.53Hz, 2H), 7.25- 7.32 (m, 2H), 7.47-7.56 (m, 2H), 8.39-8.45 (m, 1H).

By compound 9 (200mg, 503 μm of ol, 1.0 equivalents), tributyl (1- ethoxy ethylenes base) tin (364mg, 1.0mmol, 2.0 equivalents) and Pd (PPh₃)₄(58mg, 50 μm of ol, the mixture nitrogen in 0.1 equivalent) Yu dioxanes (5mL) Deaerate and purify 3 times.After stirring 16h at 100 DEG C, by reactant mixture distribution between water (15mL) and EtOAc (15mL). Wash, organic phase separation through Na with water (15mL)₂SO₄Dry, filter and concentrate under reduced pressure.Residue is dissolved in In MeOH (10mL) and add dense HCl (0.5mL).Mixture 1h is stirred at 15 DEG C and removes solvent in a vacuum.It is logical Preparative TLC (100%EtOAc) purifying residues are crossed, obtain compound 10 (130mg, 361 μm of ol, the yield in oily 72%)：¹H NMR (400MHz, CDCl₃) δ 2.20 (s, 3H), 2.36 (s, 3H), 2.60 (s, 3H), 2.71 (s, 3H), 5.45 (s, 2H), 7.18 (d, J=8.28Hz, 2H), 7.26-7.36 (m, 2H), 7.96 (d, J=8.28Hz, 2H), 8.43 (d, J= 1.88Hz, 1H).

NCS is added into solution of the compound 10 (130mg, 361 μm of ol, 1.0 equivalents) in carbon tetrachloride (10mL) (72mg, 541 μm of ol, 1.5 equivalents) and p-methyl benzenesulfonic acid (6.2mg, 36 μm of ol, 0.1 equivalent).Mixture is stirred at 70 DEG C 3h.LC/MS shows that 10 are consumed completely.Under reduced pressure concentrated reaction mixture and by preparation HPLC purify residue, Obtain the chloro- 1- of 2- (4- ((6- (the different diazole -4- bases of 3,5- dimethyl) -2- methyl isophthalic acid H- imidazos [4,5- of white solid-like B] pyridine -1- bases) methyl) phenyl) ethyl ketone (example 6) (20mg, 50 μm of ol, yield 14%, purity 98%)：¹H NMR (400MHz, DMSO-d₆) δ 2.22 (s, 3H), 2.40 (s, 3H), 2.59 (s, 3H), 5.16 (s, 2H), 5.67 (s, 2H), 7.35 (d, J=8.28Hz, 2H), 7.95 (d, J=8.41 Hz, 2H), 8.00 (d, J=2.01Hz, 1H), 8.36 (d, J=2.01Hz, 1H)；ESI m/z 395.0[M+1]⁺。

Example 7：Prepare 3,5- dimethyl -4- (2- methyl isophthalic acids-(4- (oxirane -2- ylmethyls) benzyl) -1H- imidazos [4,5-b] pyridine -6- base) isoxazoles

By compound 9 (200mg, 503 μm of ol, 1.0 equivalents), allyl tributyltin, (333mg, 1.0mmol, 2.0 work as Amount) and Pd (PPh₃)₄(58mg, 50 μm of ol, the mixture in 0.1 equivalent) Yu dioxanes (3mL) are deaerated and purified 3 times with nitrogen. Then the stirring reaction mixture 16h at 100 DEG C.After cooling, by mixture distribution water (20mL) and EtOAc (20mL) it Between.Wash, organic phase separation through Na with water (20mL)₂SO₄Dry, filter and concentrate under reduced pressure.Pass through column chromatography (50-100%EtOAc/PE) purifies residue, obtains the compound 11 (130mg, 363 μm of ol, yield 72%) in oily：¹H NMR (400MHz, CDCl₃) δ 2.19 (s, 3H), 2.36 (s, 3H), 2.74 (s, 3H), 3.39 (d, J=6.27Hz, 2H), 5.00- 5.14 (m, 2H), 5.29-5.42 (m, 2H), 5.86-6.00 (m, 1H), 7.05 (d, J=7.91Hz, 2H), 7.20 (d, J= 7.78Hz, 2H), 7.28-7.31 (m, 1H), 8.41 (d, J=1.76Hz, 1H).

At 10 DEG C, added into solution of the compound 11 (120mg, 334 μm of ol, 1 equivalent) in DMSO (1.5mL) NBS (89mg, 502 μm of ol, 1.5 equivalents).Mixture 20min is stirred at 10 DEG C, then adds DBU (101mg, 2 equivalents). Mixture 30min is stirred at 10 DEG C, reaction then is quenched with salt solution (5mL).Gained is collected by filtration to precipitate, is washed with water simultaneously And it is dried in a vacuum.Brown solid is purified by preparation HPLC, obtains 3, the 5- dimethyl -4- (2- of white solid-like Methyl isophthalic acid-(4- (oxirane -2- ylmethyls) benzyl) -1H- imidazos [4,5-b] pyridine -6- base) isoxazoles (example 7) (20mg, yield 15%).¹H NMR (400MHz, methanol-d₄)：δ 2.21 (s, 3H) 2.39 (s, 3H) 2.54 (dd, J=4.96, 2.70Hz, 1H) 2.72 (s, 3H) 2.74-2.81 (m, 2H) 2.86-2.93 (m, 1H) 3.09-3.14 (m, 1H) 5.56 (s, 2H) 7.18 (d, J=8.03Hz, 2H) 7.31 (d, J=8.16Hz, 2H) 7.82 (d, J=2.01Hz, 1H) 8.34 (d, J=2.01Hz, 1H)；ESI m/z 374.1[M+H]⁺。

Example 8：Suppress four acetylation histone H 4s and combine indivedual BET bromines domains

It is overexpressed by protein clone and with 6 × His of N-terminal labels, then passes in succession through nickel affinity chromatography, size exclusion color Spectrum purifying.In simple terms, expressed and carried with the recombinant of N-terminal nickel affinity labeling bromine domain of the coding from Brd2, Brd3, Brd4 Body converts e. coli bl21 (DE3) cell.Cell culture is cultivated to suitable density at 37 DEG C under earthquake and is used in combination IPTG overnight inductions.The supernatant for having dissolved cell is loaded on Ni-IDA posts and purified.The protein that will be eluted Merge, concentrate and further purified by size exclusion chromatography.The part for representing monomeric protein is merged, concentrate, is divided into Equal portions, and be frozen at -80 DEG C for use in subsequent experimental.

By homogeneous time-resolved fluorescence resonance energy transmission () method confirms four acetylation histone H 4s and BET The combination of bromine domain.The bromine domain (200nM) of N-terminal His marks and four acetylation histone H 4 peptides of biotin labeling (25-50nM, Mi Libo (Millipore)) is in streptavidin (the Cisbio catalog number (Cat.No.)s marked through europium cryptate In white 96 holes in the presence of the anti-His antibody of monoclonal (Cisbio catalog number (Cat.No.) 61HISXLB) 610SAKLB) and through XL665 marked Cultivated in microtiter plate (Greiner).On inhibition analysis, in these reactants into the DMSO of 0.2% ultimate density Add the test compound Jing Guo serial dilution.For the every kind of concentration tested, duplicate hole is used.Final buffer solution Concentration be 30mM HEPES pH 7.4,30mM NaCl, 0.3mM CHAPS, 20mM phosphate pH 7.0,320mM KF, 0.08%BSA.After cultivating 2h at room temperature, with SynergyH4 plate reader (uncle rises (Biotek)) measurement under 665 and 620nm Fluorescence.Relative to 620nm fluorescence, reduced in 665nm, show binding inhibition activity.IC is determined from dose-effect curve₅₀ Value.

IC₅₀Compound of the value less than or equal to 0.3 μM is considered as highly active (+++)；IC₅₀Value is between 0.3 and 3 μM Between compound be considered as very active (++)；IC₅₀Compound of the value between 3 and 30 μM is considered as active (+).

Table 2：Suppress the combination of four acetylation histone H 4s and Brd4 bromines domain 1 (BRD4 (1)), as measured by FRET

Example 9：Covalent bond is on breeding persistent influence

By MV4-11 cells (CRL-9591) with 5 × 10⁴The density of individual cells/well be coated in 96 hole flat undersides and The non-covalent control compound of covalently contrast of IC90 concentration is used in IMDM culture mediums containing 10%FBS and penicillin/streptomycin Or DMSO (0.1%) processing.For every kind of concentration, triplicate hole is used；And use the hole conduct pair only containing culture medium According to.By plate at 37 DEG C, 5%CO₂Lower cultivation 24h, removes compound, is replaced with culture medium afterwards, and 24,48 and after removing 72 hours, water-based single solution (Pu Luomaige (Promega)) of Cell Titer by adding from 20 μ L to each hole measured Breed and at 37 DEG C, 5%CO₂Under cultivate 3-4h again.Absorbance is read in spectrophotometer and passing through under 490nm After the signal correction background for subtracting blank well, the cell titer percentage relative to the cell by DMSO processing is calculated.Make IC50 values are calculated with GraphPad Prism softwares.

Table 3：Covalent bond is on breeding persistent influence

Fig. 1 shows propagation persistent influence of the covalent bond on example 1 and 4.

Example 10：Persistent influence that covalent bond suppresses on MYC and BCL2

By MV4-11 cells (CRL-9591) with 2.5 × 10⁴The density of individual cells/well is coated in 96 hole U-shaped base plates simultaneously And the test compound or DMSO of progressive concentration are used in the IMDM culture mediums containing 10%FBS and penicillin/streptomycin (0.1%) handle, and 4 are cultivated at 37 DEG C, remove compound afterwards, replaced with culture medium and 4,6 and 24 after removing Hour, collect cell.For every kind of concentration, triplicate hole is used.Cell pelletization is made by centrifugation and uses mRNA Catcher PLUS kits are collected according to the specification of manufacturer.Then institute is used in the quantitative real-time PCR reactions of one-step method The mRNA by elution of separation, uses RNA UltraSense^TMOne-step method kit (life technology (Life Technologies component)) and Applied Biosystems, Inc. for cMYC and cyclophilinPrimer-probe. Real-time PCR plate is in ViiA^TMRun on 7 real-time PCR machines (Applied Biosystems, Inc.), analyze data, by cMYC's and BCL2 Ct values standardize for internal contrast, it is then determined that each sample is expressed relative to the multiple of control.

Fig. 2 shows persistent influence that covalent bond suppresses on the MYC and BCL2 of example 1.

Example 11：Analyzed for monitoring with the covalently bound thermal migration of BET bromine domains

By 5 μM of purified bromine domain protein white matters with 5 ×Orange (molecular phycobiliprotein complexes (Molecular Probes)) together with 20mM HEPES pH 7.4,100mM NaCl ultimate density in 100 μM of compounds or DMSO (0.2%) cultivated in the presence of in quick 96 hole optical sheet (Applied Biosystems, Inc.).Sample is cultivated at room temperature 30 minutes Or 4 hours, and gradually rise to 95 DEG C from 25 DEG C in ViiA7 real-time PCR machines (Applied Biosystems, Inc.).Analysis institute Obtain fluorescence data and using Protein Thermal Shift^TMSoftware v1.0 (life technology) calculates melting temperature.Thermal migration Indicate inhibitor and protein covalent bond.

Fig. 3 shows the thermal migration data of example 1 and 4, it was demonstrated that compound covalently combines.

Example 12：Suppress the cMYC expression in cancerous cell line

By MV4-11 cells (CRL-9591) with 2.5 × 10⁴The density of individual cells/well is coated in 96 hole U-shaped base plates simultaneously And the test compound or DMSO of progressive concentration are used in the IMDM culture mediums containing 10%FBS and penicillin/streptomycin (0.1%) handle, and 3h is cultivated at 37 DEG C.For every kind of concentration, the hole of three repetitions is used.Cell ball is made by centrifugation It is granulated and is collected using mRNA Catcher PLUS kits according to the specification of manufacturer.Then it is quantitatively real in one-step method When PCR reactions in using the separated mRNA by elution, use RNAUltraSense^TMOne-step method kit (life technology (Life Technologies)) component and Applied Biosystems, Inc. for cMYC and cyclophilinPrimer- Probe.Real-time PCR plate is in ViiA^TMRun on 7 real-time PCR machines (Applied Biosystems, Inc.), analyze data, by cMYC Ct Value standardizes for internal contrast, it is then determined that each sample is expressed relative to the multiple of control.

Table 5：Suppress the c-myc activity in mankind's AML MV4-11 cells

Example number	C-myc activity	Example number	C-myc activity	Example number	C-myc activity	Example number	C-myc activity
								1	+	2	+	3	+	4	++
5	++	-	-	-	-	-	-

Example 13：Suppress the cell propagation in cancerous cell line

By MV4-11 cells (CRL-9591) with 5 × 10⁴The density of individual cells/well be coated in 96 hole flat undersides and Test compound with progressive concentration or DMSO (0.1%) place in IMDM culture mediums containing 10%FBS and penicillin/streptomycin Reason.For every kind of concentration, the hole of three repetitions is used；And the hole only containing culture medium is used as control.By plate at 37 DEG C, 5%CO₂Lower cultivation 72h, the 20 μ L water-based single solution (Pu Luomaige of CellTiter are then added into each hole (Promega)) and at 37 DEG C, 5%CO₂Under cultivate 3-4h again.Under 490nm in spectrophotometer read absorbance and After the signal correction background by subtracting blank well, the cell titer percentage relative to the cell by DMSO processing is calculated Than.IC is calculated using GraphPad Prism softwares₅₀Value.

Table 5：Suppress the cell propagation in mankind's AML MV-4-11 cells

Example 14：Suppress hIL-6mRNA transcriptions

By human leukemia monocyte lymthoma U937 cells (CRL-1593.2) with 3.2 × 10⁴Individual cells/well it is close Degree is coated in the 100 μ L RPMI-1640 containing 10%FBS and penicillin/streptomycin in 96 orifice plates, and in 60ng/mL In 5%CO at 37 DEG C in PMA (phorbol -13- myristinate -12- acetic acid esters)₂In continue to be divided into macrophage in 3 days, Then compound is added.Cell pre-processes 1h with the test compound of progressive concentration in 0.1%DMSO, is then come from 1 μ g/mL The lipopolysaccharides of Escherichia coli stimulates.For every kind of concentration, the hole of three repetitions is used.By cell at 37 DEG C, 5%CO₂Lower cultivation 3h, then collect cell.When collecting, remove culture medium and rinse cell in 200uL PBS.Use mRNA Catcher PLUS kits, cell is collected according to the specification of manufacturer.Then using by washing in the quantitative real-time PCR reactions of one-step method De- mRNA, uses RNAUltraSense^TMThe component of one-step method kit (life technology) and for hIL-6 and cyclophilin Applied Biosystems, Inc.Primer-probe.Real-time PCR plate is in ViiA^TM7 real-time PCR machines (apply biology department System company) on run, analyze data, hIL-6 Ct values are standardized for internal contrast, it is then determined that each sample relative to The multiple expression of control.

Table 6：Suppress hIL-6mRNA transcriptions

Example number

IL-6 activity

Example number

IL-6 activity

Example number

IL-6 activity

Example number

IL-6 activity

1

+

2

+

3

++

4

++

Example 15：Suppress hIL-17mRNA transcriptions

Human peripheral blood mononuclear cells are applied into paving (2.0 × 10⁵Individual cells/well) in 96 orifice plates contain 20ng/mlIL-2 In 45 μ L OpTimizer T cells amplification culture mediums (life technology) of penicillin/streptomycin.By cell progressive concentration Test compound or DMSO (0.1%) processing, and at 37 DEG C, 5%CO₂Lower cultivation 1h, then adds 10 μ in the medium G/ml 10 × storing solution OKT3 antibody.For every kind of concentration, triplicate hole is used.By cell at 37 DEG C, 5%CO₂Under 6h is cultivated, then collects cell.When collecting, by making cell pelletization 5min with 800rpm centrifugations.Use mRNA Catcher PLUS kits, cell is collected according to the specification of manufacturer.Then make in the quantitative real-time PCR reactions of one-step method With the separated mRNA by elution, RNAUltraSense is used^TMThe component and use of one-step method kit (life technology) In hIL-17 and cyclophilin Applied Biosystems, Inc.Primer-probe.Real-time PCR plate is in ViiA^TM7 real-time PCR Run, analyze data, hIL-17 Ct values are standardized for internal contrast, then really on machine (Applied Biosystems, Inc.) Fixed each unknown sample induces relative to the multiple of control.

Example 16：Using MV4-11 cells, the body in nude mouse strain acute myelogenous leukemia heteroplastic transplantation model Interior effect：

MV4-11 cells (ATCC) are made to be grown under standard cell culture conditions and to (NCr) nu/nu of 6 to 7 week old 5 × 10 in the μ L PBS+100 μ L matrigels of left lower quadrant side injection 100 of fiso1 strain female mices⁶Individual cell/animal. The about the 18 to 21st day after the injection of MV4-11 cells, 300mm is arrived based on average about 100³Gross tumor volume ((L × W × H)/2) Mouse is grouped at random.Mouse is by following dosage regimen with every kg body weight 10mL dose volumes orally administration EA006 preparations In compound：5 arrive 120mg/kg b.i.d and/or q.a. continuous dosing regimens；85mg/kg q.d. are arrived with 2.5, to 5 days Stop 2 days；100mg/kg q.d., stopped 3 days to 4 days；135mg/kg q.d., stopped 4 days to 3 days；180mg/kg, stopped 5 days to 2 days； And 240mg/kg, to 1 day dosage regimen for stopping 6 days.Since administration phase, every other day with regard to carrying out tumour with electronics microcaloire chi Measure and measure body weight.Relative to mediator control-animal compare mean tumour volume, Tumor growth inhibition (TGI) percentage with And body weight changes %.The comparison calculated in Excel between average value, statistical analysis and each group is examined using student t.

Example 17：Assess target spot effect (Target Engagement)

MV4-11 and MM1.s cells (ATCC) are made to be grown under standard cell culture conditions and to 6 to 7 week old (NCr) 5 × 10 in the μ L PBS+100 μ L matrigels of left lower quadrant side injection 100 of nu/nu fiso1 strains female mice⁶It is individual thin Born of the same parents/animal.The about the 28th day after the injection of MV4-11 and MM1.s cells, based on average about 500mm³Gross tumor volume ((L × W × H)/2) be grouped mouse at random.In the EA006 preparations that every kg body weight 10mL dose volumes are given to its mouse oral Compound, and upon administration 3,6,12,24h collect tumour, for Bcl2 and c-myc gene expression analysis as PD biology marks Note.

Example 18：Effect inside in MS experimental autoimmune encephalomyelitis (EAE) model

Experimental autoimmune encephalomyelitis (EAE) is the CNS autoimmune diseases of T cell mediation, and it is more with the mankind Hair property sclerosis (MS) has many common clinics and Histopathological Characteristics.EAE is the most frequently used MS animal models.Th1 and The T cell of Th17 pedigrees, which is shown, can induce EAE.For Th1 and Th17 differentiation it is very crucial or as caused by these T cells cell The factor IL-23, IL-6 and IL-17 EAE development in play a part of key and nonredundancy.Therefore, target these cells because The caused medicine of son may have treatment MS treatment potential.

From immunization time, with 50 to 125mg/kg b.i.d. to EAE mouse administration Formulas I or Formula II compound to evaluate Antiphlogistic activity.In this model, MOG is passed through_35-55/ CFA is immune and injection pertussis toxin lures in female C57B1/6 mouse EAE is sent out.

Consider from the practice of this specification and inventions disclosed herein, other embodiments of the invention are to this area Those of ordinary skill for will be obvious.Wish only to be considered as specification and example exemplary, and the present invention True scope and spirit specified by following claims.

Claims

1. a kind of compound of formula I,

Wherein：

R₄Selected from hydrogen, optionally by 1 to 5 independently selected from R₅Group substitution alkyl (C₁-C₁₀), carbocyclic ring (C₃-C₁₀) and Heterocycle (C₂-C₁₀)；

Y is selected from-N- ,-CH- and-CNH₂-。

2. a kind of Formula II compound,

Wherein：

Z is selected from hydrogen and amino.

3. the compound according to claim 1 or claim 2, wherein R₁Selected from optionally by 1 to 5 independently selected from R₅Group substitution carbocyclic ring (C₅-C₁₀)。

4. the compound according to any claim in Claim 1-3, wherein R₁Selected from optionally by 1 to 5 independences Ground is selected from R₅Group substitution phenyl.

5. the compound according to any claim in claim 1 to 4, wherein R₁Selected from by 1 to 5 independently selected from R₅Group substitution phenyl.

6. the compound according to any claim in claim 1 to 5, wherein R₁Selected from by 1 to 5 independently selected from Epoxides, alkyl (C₁-C₆), halogen and ketone (C₁-C₆) group substitution phenyl, these groups each can optionally by Oxirane, hydrogen, F, Br and/or Cl substitution.

7. the compound according to any claim in claim 1 to 6, wherein R₁Selected from by 1 to 5 independently selected from Oxirane, methyl, ethyl, F and acetyl group group substitution phenyl, these groups each can be optionally by oxirane Substitute with Cl.

8. the compound according to any claim in claim 1 to 7, wherein R₁Selected from by oxirane, methyl epoxy Ethane, halogen ketone (C₁-C₆) and/or alkylhalide group (C₁-C₆) substitution phenyl.

9. the compound according to any claim in claim 1 to 8, wherein R₁It is selected from：

10. the compound according to any claim in claim 1 to 9, wherein R₁It is selected from：

Wherein benzyl ring is optionally further optionally substituted by halogen.

11. the compound according to any claim in claim 1 to 10, wherein R₁It isIts Middle benzyl ring is optionally further by 1 to 4 independently selected from R₅Group substitution.

12. the compound according to any claim in claim 1 to 11, wherein R₁It isIts Middle benzyl ring is optionally further optionally substituted by halogen.

13. the compound according to any claim in claim 1 to 12, wherein R₁It is

14. the compound according to any claim in claim 1 to 13, wherein R₁It is selected from：

It is optionally by 1 to 4 independently selected from R₅Group substitution.

15. the compound according to any claim in claim 1 to 14, wherein R₁It is selected from：

16. the compound according to any claim in claim 1 to 15, wherein R₁It is selected from：

17. the compound according to claim 1 or claim 2, wherein R₁Selected from optionally by 1 to 5 independently selected from R₅Group substitution heterocycle (C₂-C₁₀)。

18. according to the compound described in any claim in claim 1,2 and 17, wherein R₁Selected from by oxirane, methyl Oxirane, halogen ketone (C₁-C₆) and/or alkylhalide group (C₁-C₆) substitution 5-6 circle heterocycles.

19. the compound according to any claim in claim 1 to 18, wherein R₂It is methyl and R₃Selected from optional Alkyl (the C that ground is substituted by halogen and hydroxyl₁-C₆)。

20. the compound according to any claim in claim 1 to 19, wherein R₂And R₃It is methyl.

21. the compound according to any claim in claim 1 to 20, wherein R₄Selected from hydrogen and optionally by 1 to 5 It is individual independently selected from R₅Group substitution alkyl (C₁-C₆)。

22. the compound according to any claim in claim 1 to 21, wherein R₄It is hydrogen.

23. the compound according to any claim in claim 1 to 21, wherein R₄Selected from only optionally by 1 to 5 On the spot it is selected from R₅Group substitution alkyl (C₁-C₆)。

24. according to the compound described in any claim in claim 1 to 21 and 23, wherein R₄It is methyl.

25. the compound according to any claim in claim 1 to 19, wherein R₄Selected from only optionally by 1 to 5 On the spot it is selected from R₅Group substitution heterocycle (C₂-C₆)。

26. the compound according to any claim in claim 1 to 19, wherein R₄Selected from only optionally by 1 to 5 On the spot it is selected from R₅Group substitution carbocyclic ring (C₃-C₁₀)。

27. the compound according to any claim in claim 1 to 26, wherein each R₅Independently selected from deuterium, epoxy Compound, alkyl (C₁-C₆), amino ,-NHC (O) NH- alkyl (C₁-C₆), halogen, acid amides ,-CF₃、-CN、-N₃, ketone (C₁-C₆)、-S (O) alkyl (C₁-C₄)、-SO₂Alkyl (C₁-C₆) and sulfanyl (C₁-C₆)。

28. the compound according to any claim in claim 1 to 27, wherein Y are-CH-.

29. the compound according to any claim in claim 1 to 27, wherein Y are-N-.

30. the compound according to any claim in claim 1 to 27, wherein Y are-C (NH₂)-。

31. compound according to claim 1, wherein X are-CH₂-。

32. compound according to claim 1, wherein Z are hydrogen.

33. compound according to claim 1, wherein Z are-NH₂。

34. the compound according to claim 1 or claim 2, wherein the Formulas I or Formula II compound are selected from：

4- (1- { [4- (2- chloroethyls) phenyl] methyl } -2- methyl isophthalic acid H- imidazos [4,5-b] pyridine -6- bases) -3,5- diformazans Base -1,2- oxazoles；

The chloro- 1- of 2- (4- { [6- (dimethyl -1,2- oxazole -4- bases) -2- methyl isophthalic acid H- imidazo [4,5-b] pyridines -1 base] first Base } phenyl) second -1- ketone；

Its stereoisomer, dynamic isomer, pharmaceutically acceptable salt or hydrate.

A kind of 35. pharmaceutical composition, comprising the compound according to any claim in Claim 1-3 4 and pharmaceutically Acceptable supporting agent.

A kind of 36. method for being used to suppress BET protein functions, comprising administration therapeutically effective amount according to Claim 1-3 4 Compound or pharmaceutical composition according to claim 35 described in middle any claim.

37. a kind of method for treating the LADA relevant with BET protein or inflammatory conditions, effective comprising administration treatment The compound according to any claim in Claim 1-3 4 of amount or drug regimen according to claim 35 Thing.

38. according to the method for claim 37, wherein the LADA or inflammatory conditions are selected from acute disseminated Encephalomyelitis, agammaglobulinemia, anaphylactia, stiff property spondylitis, the anti-TBM ephritis of anti-GBM/, anti-phosphatide synthesis Sign, LADA alpastic anemia, oneself immunity hepatitis, Autoimmune Inner Ear Disease, autoimmune myocarditis, Autoimmune pancreatitis, autoimmune retinopathy, autoimmune thrombocytopenic purpura, Behcet's disease (Behcet' S Disease), bullous pemphigoid, castleman's disease (Castleman's Disease), chylous diarrhea, Qiu-apply Er Shi it is comprehensive Simulator sickness (Churg-Strauss syndrome), Crohn's disease (Crohn's Disease), Ke's radicular syndrome (Cogan's Syndrome), dry eye syndrome, primary mixed type cryoglobulinemia, dermatomyositis, devic's disease (Devic's Disease), encephalitis, eosinophilic esophagitis, eosinophilic fasciitis, erythema nodosum, giant cell arteritis, glomerulonephritis, Goodpasture's syndrome (Goodpasture's syndrome), granulomatous Polyangiitis (Wegener (Wegener's)), Graves disease (Graves'Disease), Guillain-Barre＆1＆ syndrome (Guillain-Barre syndrome), Hashimoto first Shape adenositis (Hashimoto's thyroiditis), hemolytic anemia, purpura,Henoch-Schonlein (Henoch-Schonlein Purpura), idiopathic pulmonary fibrosis, IgA nephrosis, inclusion body myositis, type i diabetes, interstitial cystitis, Kawasaki disease (Kawasaki's Disease), leukocytoclastic angiitis, lichen planus, lupus (SLE), microscopic polyangitis, It is multiple sclerosis, myasthenia gravis, myositis, optic neuritis, pemphigus, POEMS syndromes, PAN, primary Property biliary cirrhosis, psoriasis, arthritic psoriasis, pyoderma gangraenosum, relapsing polychondritis, rheumatoid joint Inflammation, sarcoidosis, chorionitis, Sjogren syndrome (Sjogren's syndrome), takayasu's arteritis (Takayasu's Arteritis), transverse myelitis, ulcerative colitis, uveitis and leucoderma.

A kind of 39. acute or chronic non-self immune inflammatory illness treated characterized by IL-6 and/or IL-17 imbalance Method, the compound according to any claim in Claim 1-3 4 comprising administration therapeutically effective amount or according to Pharmaceutical composition described in claim 35.

40. according to the method for claim 39, wherein the acute or chronic non-self immune inflammatory illness is selected from Nasosinusitis, pneumonia, osteomyelitis, gastritis, enteritis, gingivitis, appendicitis, irritable colon syndrome, tissue transplantation rejection react, are slow It is property obstructive lung disease (COPD), septic shock, osteoarthritis, acute gout, ALI, acute renal failure, burn, conspicuous Family name reacts (Herxheimer reaction) and the SIRS relevant with viral infection.

41. according to the method for claim 39, wherein the acute or chronic non-self immune inflammatory illness is selected from Rheumatoid arthritis (RA) and multiple sclerosis (MS).

42. a kind of treat the cancer relevant with overexpression, transposition, amplification or the restructuring for suppressing sensitive myc families cancer protein to BET The method of disease, the compound or root according to any claim in Claim 1-3 4 comprising administration therapeutically effective amount According to the pharmaceutical composition described in claim 35.

43. a kind of method for treating the cancer relevant with the overexpression of BET protein, transposition, amplification or restructuring, is controlled comprising administration Treat the compound according to any claim in Claim 1-3 4 of effective dose or medicine according to claim 35 Compositions.

44. one kind treatment adjusts the cancer of oncogene dependent on pTEFb (Cdk9/ cyclin T) and BET protein Method, the compound according to any claim in Claim 1-3 4 comprising administration therapeutically effective amount or according to Pharmaceutical composition described in claim 35.

45. a kind of method for treating the cancer relevant with BET response genes CDK6, Bcl2, TYRO3, MYB and hTERT up-regulation, Compound according to any claim in Claim 1-3 4 comprising administration therapeutically effective amount or according to claim Pharmaceutical composition described in 35.

46. a kind of method for treating the cancer relevant with the gene adjusted by super enhancer, includes administration therapeutically effective amount Compound or pharmaceutical composition according to claim 35 according to any claim in Claim 1-3 4.

A kind of 47. method for treating the cancer sensitive to BET inhibitory action, comprising administration therapeutically effective amount according to claim Compound or pharmaceutical composition according to claim 35 in 1 to 34 described in any claim.

48. a kind of treat to the side with immunotherapy, hormonal deprivation and/or the resistant cancer of regimen chemotherapy Method, the compound according to any claim in Claim 1-3 4 comprising administration therapeutically effective amount or according to right It is required that the pharmaceutical composition described in 35.

49. the method according to any claim in claim 36 to 48, wherein according to any in Claim 1-3 4 Compound or pharmaceutical composition according to claim 35 and other therapies, chemotherapeutant or anti-described in claim Multiplication agent combines.

50. according to the method for claim 49, wherein the therapeutic agent is selected from ABT-737, azacitidine (prick by Victor (Vidaza)), AZD1152 (Barasertib (Barasertib)), AZD2281 (olaparib (Olaparib)), AZD6244 (U.S. of department replaces Buddhist nun (Selumetinib)), BEZ235, bleomycin sulfate (Bleomycin Sulfate), bortezomib (Bortezomib) (Bortezomib (Velcade)), busulfan (Busulfan) (bridle orchid (Myleran)), camptothecine, cis-platinum, ring Phosphamide (carat sweet smell (Clafen)), CYT387, cytarabine (Ara-C), Dacarbazine (Dacarbazine), DAPT (GSI- IX), Decitabine (Decitabine), dexamethasone (Dexamethasone), (A Deli is mould for adriamycin (Doxorubicin) Plain (Adriamycin)), Etoposide (Etoposide), everolimus (Everolimus) (RAD001), Flavopiridol (Flavopiridol) (Avobenzene west ground (Alvocidib)), Jia Litepi (Ganetespib) (STA-9090), Gefitinib (Gefitinib) (rice support is celestial for (Iressa (Iressa)), idarubicin (Idarubicin), ifosfamide (Mitoxana)), IFNa2a (Recomvinated Interferon α-2a A (Roferon A)), melphalan (Melphalan) (L-Sarcolysinum (Alkeran)), plum Fill in azoles Lars and lead to (Methazolastone) (Temozolomide (temozolomide)), melbine (Metformin), rice support anthracene Quinone (Mitoxantrone) (Novantrone (Novantrone)), taxol (Paclitaxel), insoral (Phenformin), PKC412 (midostaurin (Midostaurin)), PLX4032 (Wei Luofeini (Vemurafenib)), pomalidomide (Pomalidomide) (CC-4047), metacortandracin (Prednisone) (delta pine (Deltasone)), rapamycin (Rapamycin), Revlimid (Revlimid) (lenalidomide (Lenalidomide)), Luso profit replace Buddhist nun (Ruxolitinib) (Buddhist nun of relaxing replaces by (INCB018424), Sorafenib (Sorafenib) (Nexavar (Nexavar)), SU11248 Buddhist nun (Sunitinib)), SU11274, vincaleukoblastinum (Vinblastine), vincristine (Vincristine) (Vincristinum Sulfate (Oncovin)), vinorelbine (Vinorelbine) (NVB (Navelbine)), Vorinostat (Vorinostat) And WP1130 (wearing lattice Racine (Degrasyn)) (SAHA).

51. a kind of method for treating benign proliferative or fibrotic conditions, the benign proliferative or fibrotic conditions be selected from by The group of consisting of：Benign soft tissue neoplasm, bone tumour, brain and tumor of spinal cord, eyelid and orbital tumor, granuloma, fat Knurl, meningioma, Multiple Endocrine neoplasia, nasal polyp, pituitary tumor, prolactinoma, pseudotumor cerebri, seborrheic keratosis, Polyp of stomach, thyroid nodule, pancreas capsule anything superfluous or useless, hemangioma, vocal nodule, polyp and tumour, castleman's disease, chronic Tibetan hair Disease, histiocytoma, pilar cyst, pyogenic granuloma, juvenile polyposis syndrome, idiopathic pulmonary fibrosis, kidney fiber Change, postoperative stenosis, keloid is formed, chorionitis and cardiac fibrosis, methods described include the root of administration therapeutically effective amount According to the compound described in any claim in Claim 1-3 4 or pharmaceutical composition according to claim 35.

52. a kind of treat the method for benefiting from up-regulation or the disease or illness of ApoA-I transcriptions and protein expression, administration is included The compound or according to claim 35 according to any claim in Claim 1-3 4 of therapeutically effective amount Pharmaceutical composition.

53. method according to claim 52, wherein the disease is angiocardiopathy, dyslipidemia, Atherosclerosis Change, hypercholesterolemia, metabolic syndrome and Alzheimer disease (Alzheimer's disease).

A kind of 54. method for treating the cancer relevant with virus, comprising administration therapeutically effective amount according in Claim 1-3 4 Compound or pharmaceutical composition according to claim 35 described in any claim.

55. a kind of method for treating HIV, individually or with the treatment that ART agent is combined have comprising administration The compound according to any claim in Claim 1-3 4 or medicine group according to claim 35 of effect amount Compound.

56. one kind is used to treat selected from Alzheimer disease, Parkinson's (Parkinson's disease), Huntington disease (Huntington disease), anxiety disorder, schizophrenia, Rubinstein-Taybi syndrome (Rubinstein-Taybi Syndrome) and the method for the disease of epilepsy or illness, comprising administration therapeutically effective amount according in Claim 1-3 4 Compound or pharmaceutical composition according to claim 35 described in any claim.

A kind of 57. male contraception method, comprising administration therapeutically effective amount according to any claim institute in Claim 1-3 4 The compound or pharmaceutical composition according to claim 35 stated.